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Rilonacept Reduces Gout Flares Triggered by Urate-Lowering Therapy
LONDON – Prophylactic treatment with the potent interleukin-1 inhibitor rilonacept significantly reduced the incidence of acute gout flares triggered by the initiation of urate-lowering therapy, according to data from a global phase III study reported at the annual European Congress of Rheumatology.
Patients in the 16-week trial who were randomized to receive weekly subcutaneous injections of either 80 mg or 160 mg of rilonacept (Acralyst) at the outset of standard uric acid–reducing treatment with allopurinol had significantly fewer gout flares and significantly fewer days per flare than did patients randomized to placebo, said principal investigator Dr. Essack Mitha of Newtown Clinical Research in Johannesburg, South Africa.
Further, treatment with the fusion protein, which interrupts the inflammatory cascade by attaching to and neutralizing interleukin-1, demonstrated acceptable safety and tolerability, he said.
The findings are consistent with those of a sister phase III trial in North America reported at the 2010 annual meeting of the American College of Rheumatology, he said.
The phase III, double-blind Preventive Study Against Urate-Lowering Drug-Induced Gout Exacerbations (PRE-SURGE 2) was conducted in South Africa, Germany, and Asia, and included 248 patients with gout, serum uric acid levels of 7.5 mg/dL or higher, and a history of at least two gout flares in the prior year. All of the patients were initiated on 300 mg of allopurinol daily (except those with documented renal dysfunction, who were initiated on a lower dose), and subsequently titrated to achieve target urate levels of less than 6 mg/dL, Dr. Mitha stated.
After the initial allopurinol dose, which was continued for 20 weeks, including a 4-week safety follow-up period, patients were randomized to receive 16 weekly subcutaneous injections of placebo (82 patients), 80 mg of rilonacept with a double dosing on day 1 (82 patients), or 160 mg of rilonacept with a double dosing on day 1 (84 patients). During the study, nonsteroidal anti-inflammatory drugs and oral steroids were allowed for the treatment but not for prevention of gout flares, said Dr. Mitha.
"The primary end point was the mean number of gout flares per patient through week 16. The secondary end points were the proportion of patients experiencing two or more gout flares during this period and the number of flare-days per patient," he said, adding that safety and tolerability were also assessed.
At baseline, the characteristics of the predominantly male (93%) study population were similar across all three groups, with a mean age of 51 years, a mean serum uric acid level of 9.4 mg/dL, a mean of seven gout flares in the prior year, and a mean gout flare duration of 3.8 days. A similar number of patients in the placebo and rilonacept groups completed the treatment period, Dr. Mitha reported.
With respect to the primary end point, the mean number of gout flares per patient was 101 in the placebo group, 29 in the 80-mg rilonacept group, and 28 in the 160-mg rilonacept group, which represent a significant reduction in gout flares relative to placebo, said Dr. Mitha.
"Compared with placebo, the proportion of patients who experienced more than one gout flare through week 16 was reduced by 54% in the 80-mg group and 63% in the 160-mg group," he said. The respective reductions relative to placebo in the proportion of patients experiencing two or more flares were 74% and 82%. "The mean number of gout flare days per patient was also significantly lower in the rilonacept subjects, at 4.3 and 1.9 for the 80-mg and 160-mg groups, respectively, compared with 11.2 for placebo," and significantly fewer patients in the treatment arms had flares lasting 5 days or longer, he said.
In terms of adverse events, the overall incidence was similar across the groups, and although there were more injection-site reactions in the rilonacept groups, "the reactions were generally mild, and none of the patients withdrew for that reason," Dr. Mitha said. Three patients did withdraw from the higher-dose rilonacept group for other reasons – one each for neutropenia, gout flare, and gastric cancer – "but there were no deaths and no serious adverse events related to the product," he stressed.
Together with the results of the North American PRE-SURGE 1 trial, the findings of this study are an important step in the clinical development program for rilonacept, which the U.S. Food and Drug Administration approved in February 2008 for the treatment of cryopyrin-associated periodic syndromes and Muckle-Wells syndrome in adults and children older than 12 years.
"Our results suggest that concomitant use of rilonacept during the first several months of allopurinol therapy may help avoid the acute gout flares that make it difficult for patients to maintain urate-lowering therapy," according to Dr. Mitha. Currently, standard practice includes the use of colchicine or anti-inflammatory drugs to reduce the risk of flares associated with early allopurinol, but the gastrointestinal side effects associated with colchicine in particular can be prohibitive, he said.
Because rilonacept is "very expensive" compared with standard treatment for acute gout flares, studies looking at the relative efficacy of the various treatment options are warranted before the drug should be widely used for this indication, Dr. Mitha stressed.
Dr. Mitha and his coinvestigators disclosed receiving grant/research support from Regeneron Pharmaceuticals, which manufactures rilonacept.
LONDON – Prophylactic treatment with the potent interleukin-1 inhibitor rilonacept significantly reduced the incidence of acute gout flares triggered by the initiation of urate-lowering therapy, according to data from a global phase III study reported at the annual European Congress of Rheumatology.
Patients in the 16-week trial who were randomized to receive weekly subcutaneous injections of either 80 mg or 160 mg of rilonacept (Acralyst) at the outset of standard uric acid–reducing treatment with allopurinol had significantly fewer gout flares and significantly fewer days per flare than did patients randomized to placebo, said principal investigator Dr. Essack Mitha of Newtown Clinical Research in Johannesburg, South Africa.
Further, treatment with the fusion protein, which interrupts the inflammatory cascade by attaching to and neutralizing interleukin-1, demonstrated acceptable safety and tolerability, he said.
The findings are consistent with those of a sister phase III trial in North America reported at the 2010 annual meeting of the American College of Rheumatology, he said.
The phase III, double-blind Preventive Study Against Urate-Lowering Drug-Induced Gout Exacerbations (PRE-SURGE 2) was conducted in South Africa, Germany, and Asia, and included 248 patients with gout, serum uric acid levels of 7.5 mg/dL or higher, and a history of at least two gout flares in the prior year. All of the patients were initiated on 300 mg of allopurinol daily (except those with documented renal dysfunction, who were initiated on a lower dose), and subsequently titrated to achieve target urate levels of less than 6 mg/dL, Dr. Mitha stated.
After the initial allopurinol dose, which was continued for 20 weeks, including a 4-week safety follow-up period, patients were randomized to receive 16 weekly subcutaneous injections of placebo (82 patients), 80 mg of rilonacept with a double dosing on day 1 (82 patients), or 160 mg of rilonacept with a double dosing on day 1 (84 patients). During the study, nonsteroidal anti-inflammatory drugs and oral steroids were allowed for the treatment but not for prevention of gout flares, said Dr. Mitha.
"The primary end point was the mean number of gout flares per patient through week 16. The secondary end points were the proportion of patients experiencing two or more gout flares during this period and the number of flare-days per patient," he said, adding that safety and tolerability were also assessed.
At baseline, the characteristics of the predominantly male (93%) study population were similar across all three groups, with a mean age of 51 years, a mean serum uric acid level of 9.4 mg/dL, a mean of seven gout flares in the prior year, and a mean gout flare duration of 3.8 days. A similar number of patients in the placebo and rilonacept groups completed the treatment period, Dr. Mitha reported.
With respect to the primary end point, the mean number of gout flares per patient was 101 in the placebo group, 29 in the 80-mg rilonacept group, and 28 in the 160-mg rilonacept group, which represent a significant reduction in gout flares relative to placebo, said Dr. Mitha.
"Compared with placebo, the proportion of patients who experienced more than one gout flare through week 16 was reduced by 54% in the 80-mg group and 63% in the 160-mg group," he said. The respective reductions relative to placebo in the proportion of patients experiencing two or more flares were 74% and 82%. "The mean number of gout flare days per patient was also significantly lower in the rilonacept subjects, at 4.3 and 1.9 for the 80-mg and 160-mg groups, respectively, compared with 11.2 for placebo," and significantly fewer patients in the treatment arms had flares lasting 5 days or longer, he said.
In terms of adverse events, the overall incidence was similar across the groups, and although there were more injection-site reactions in the rilonacept groups, "the reactions were generally mild, and none of the patients withdrew for that reason," Dr. Mitha said. Three patients did withdraw from the higher-dose rilonacept group for other reasons – one each for neutropenia, gout flare, and gastric cancer – "but there were no deaths and no serious adverse events related to the product," he stressed.
Together with the results of the North American PRE-SURGE 1 trial, the findings of this study are an important step in the clinical development program for rilonacept, which the U.S. Food and Drug Administration approved in February 2008 for the treatment of cryopyrin-associated periodic syndromes and Muckle-Wells syndrome in adults and children older than 12 years.
"Our results suggest that concomitant use of rilonacept during the first several months of allopurinol therapy may help avoid the acute gout flares that make it difficult for patients to maintain urate-lowering therapy," according to Dr. Mitha. Currently, standard practice includes the use of colchicine or anti-inflammatory drugs to reduce the risk of flares associated with early allopurinol, but the gastrointestinal side effects associated with colchicine in particular can be prohibitive, he said.
Because rilonacept is "very expensive" compared with standard treatment for acute gout flares, studies looking at the relative efficacy of the various treatment options are warranted before the drug should be widely used for this indication, Dr. Mitha stressed.
Dr. Mitha and his coinvestigators disclosed receiving grant/research support from Regeneron Pharmaceuticals, which manufactures rilonacept.
LONDON – Prophylactic treatment with the potent interleukin-1 inhibitor rilonacept significantly reduced the incidence of acute gout flares triggered by the initiation of urate-lowering therapy, according to data from a global phase III study reported at the annual European Congress of Rheumatology.
Patients in the 16-week trial who were randomized to receive weekly subcutaneous injections of either 80 mg or 160 mg of rilonacept (Acralyst) at the outset of standard uric acid–reducing treatment with allopurinol had significantly fewer gout flares and significantly fewer days per flare than did patients randomized to placebo, said principal investigator Dr. Essack Mitha of Newtown Clinical Research in Johannesburg, South Africa.
Further, treatment with the fusion protein, which interrupts the inflammatory cascade by attaching to and neutralizing interleukin-1, demonstrated acceptable safety and tolerability, he said.
The findings are consistent with those of a sister phase III trial in North America reported at the 2010 annual meeting of the American College of Rheumatology, he said.
The phase III, double-blind Preventive Study Against Urate-Lowering Drug-Induced Gout Exacerbations (PRE-SURGE 2) was conducted in South Africa, Germany, and Asia, and included 248 patients with gout, serum uric acid levels of 7.5 mg/dL or higher, and a history of at least two gout flares in the prior year. All of the patients were initiated on 300 mg of allopurinol daily (except those with documented renal dysfunction, who were initiated on a lower dose), and subsequently titrated to achieve target urate levels of less than 6 mg/dL, Dr. Mitha stated.
After the initial allopurinol dose, which was continued for 20 weeks, including a 4-week safety follow-up period, patients were randomized to receive 16 weekly subcutaneous injections of placebo (82 patients), 80 mg of rilonacept with a double dosing on day 1 (82 patients), or 160 mg of rilonacept with a double dosing on day 1 (84 patients). During the study, nonsteroidal anti-inflammatory drugs and oral steroids were allowed for the treatment but not for prevention of gout flares, said Dr. Mitha.
"The primary end point was the mean number of gout flares per patient through week 16. The secondary end points were the proportion of patients experiencing two or more gout flares during this period and the number of flare-days per patient," he said, adding that safety and tolerability were also assessed.
At baseline, the characteristics of the predominantly male (93%) study population were similar across all three groups, with a mean age of 51 years, a mean serum uric acid level of 9.4 mg/dL, a mean of seven gout flares in the prior year, and a mean gout flare duration of 3.8 days. A similar number of patients in the placebo and rilonacept groups completed the treatment period, Dr. Mitha reported.
With respect to the primary end point, the mean number of gout flares per patient was 101 in the placebo group, 29 in the 80-mg rilonacept group, and 28 in the 160-mg rilonacept group, which represent a significant reduction in gout flares relative to placebo, said Dr. Mitha.
"Compared with placebo, the proportion of patients who experienced more than one gout flare through week 16 was reduced by 54% in the 80-mg group and 63% in the 160-mg group," he said. The respective reductions relative to placebo in the proportion of patients experiencing two or more flares were 74% and 82%. "The mean number of gout flare days per patient was also significantly lower in the rilonacept subjects, at 4.3 and 1.9 for the 80-mg and 160-mg groups, respectively, compared with 11.2 for placebo," and significantly fewer patients in the treatment arms had flares lasting 5 days or longer, he said.
In terms of adverse events, the overall incidence was similar across the groups, and although there were more injection-site reactions in the rilonacept groups, "the reactions were generally mild, and none of the patients withdrew for that reason," Dr. Mitha said. Three patients did withdraw from the higher-dose rilonacept group for other reasons – one each for neutropenia, gout flare, and gastric cancer – "but there were no deaths and no serious adverse events related to the product," he stressed.
Together with the results of the North American PRE-SURGE 1 trial, the findings of this study are an important step in the clinical development program for rilonacept, which the U.S. Food and Drug Administration approved in February 2008 for the treatment of cryopyrin-associated periodic syndromes and Muckle-Wells syndrome in adults and children older than 12 years.
"Our results suggest that concomitant use of rilonacept during the first several months of allopurinol therapy may help avoid the acute gout flares that make it difficult for patients to maintain urate-lowering therapy," according to Dr. Mitha. Currently, standard practice includes the use of colchicine or anti-inflammatory drugs to reduce the risk of flares associated with early allopurinol, but the gastrointestinal side effects associated with colchicine in particular can be prohibitive, he said.
Because rilonacept is "very expensive" compared with standard treatment for acute gout flares, studies looking at the relative efficacy of the various treatment options are warranted before the drug should be widely used for this indication, Dr. Mitha stressed.
Dr. Mitha and his coinvestigators disclosed receiving grant/research support from Regeneron Pharmaceuticals, which manufactures rilonacept.
FROM THE ANNUAL EUROPEAN CONGRESS OF RHEUMATOLOGY
Major Finding: The interleukin-1 inhibitor rilonacept reduced the rate of acute gout flares through 16 weeks of treatment by 54% in patients receiving an 80-mg injection and 63% in patients getting 160 mg.
Data Source: A 16-week, phase III, double-blind, randomized trial evaluating the impact of weekly subcutaneous injections of rilonacept on gout flares relative to placebo in 248 patients being treated with allopurinol.
Disclosures: Dr. Mitha and his coinvestigators disclosed receiving grant/research support from Regeneron Pharmaceuticals, which manufactures rilonacept.
Rilonacept Reduces Gout Flares Triggered by Urate-Lowering Therapy
LONDON – Prophylactic treatment with the potent interleukin-1 inhibitor rilonacept significantly reduced the incidence of acute gout flares triggered by the initiation of urate-lowering therapy, according to data from a global phase III study reported at the annual European Congress of Rheumatology.
Patients in the 16-week trial who were randomized to receive weekly subcutaneous injections of either 80 mg or 160 mg of rilonacept (Acralyst) at the outset of standard uric acid–reducing treatment with allopurinol had significantly fewer gout flares and significantly fewer days per flare than did patients randomized to placebo, said principal investigator Dr. Essack Mitha of Newtown Clinical Research in Johannesburg, South Africa.
Further, treatment with the fusion protein, which interrupts the inflammatory cascade by attaching to and neutralizing interleukin-1, demonstrated acceptable safety and tolerability, he said.
The findings are consistent with those of a sister phase III trial in North America reported at the 2010 annual meeting of the American College of Rheumatology, he said.
The phase III, double-blind Preventive Study Against Urate-Lowering Drug-Induced Gout Exacerbations (PRE-SURGE 2) was conducted in South Africa, Germany, and Asia, and included 248 patients with gout, serum uric acid levels of 7.5 mg/dL or higher, and a history of at least two gout flares in the prior year. All of the patients were initiated on 300 mg of allopurinol daily (except those with documented renal dysfunction, who were initiated on a lower dose), and subsequently titrated to achieve target urate levels of less than 6 mg/dL, Dr. Mitha stated.
After the initial allopurinol dose, which was continued for 20 weeks, including a 4-week safety follow-up period, patients were randomized to receive 16 weekly subcutaneous injections of placebo (82 patients), 80 mg of rilonacept with a double dosing on day 1 (82 patients), or 160 mg of rilonacept with a double dosing on day 1 (84 patients). During the study, nonsteroidal anti-inflammatory drugs and oral steroids were allowed for the treatment but not for prevention of gout flares, said Dr. Mitha.
"The primary end point was the mean number of gout flares per patient through week 16. The secondary end points were the proportion of patients experiencing two or more gout flares during this period and the number of flare-days per patient," he said, adding that safety and tolerability were also assessed.
At baseline, the characteristics of the predominantly male (93%) study population were similar across all three groups, with a mean age of 51 years, a mean serum uric acid level of 9.4 mg/dL, a mean of seven gout flares in the prior year, and a mean gout flare duration of 3.8 days. A similar number of patients in the placebo and rilonacept groups completed the treatment period, Dr. Mitha reported.
With respect to the primary end point, the mean number of gout flares per patient was 101 in the placebo group, 29 in the 80-mg rilonacept group, and 28 in the 160-mg rilonacept group, which represent a significant reduction in gout flares relative to placebo, said Dr. Mitha.
"Compared with placebo, the proportion of patients who experienced more than one gout flare through week 16 was reduced by 54% in the 80-mg group and 63% in the 160-mg group," he said. The respective reductions relative to placebo in the proportion of patients experiencing two or more flares were 74% and 82%. "The mean number of gout flare days per patient was also significantly lower in the rilonacept subjects, at 4.3 and 1.9 for the 80-mg and 160-mg groups, respectively, compared with 11.2 for placebo," and significantly fewer patients in the treatment arms had flares lasting 5 days or longer, he said.
In terms of adverse events, the overall incidence was similar across the groups, and although there were more injection-site reactions in the rilonacept groups, "the reactions were generally mild, and none of the patients withdrew for that reason," Dr. Mitha said. Three patients did withdraw from the higher-dose rilonacept group for other reasons – one each for neutropenia, gout flare, and gastric cancer – "but there were no deaths and no serious adverse events related to the product," he stressed.
Together with the results of the North American PRE-SURGE 1 trial, the findings of this study are an important step in the clinical development program for rilonacept, which the U.S. Food and Drug Administration approved in February 2008 for the treatment of cryopyrin-associated periodic syndromes and Muckle-Wells syndrome in adults and children older than 12 years.
"Our results suggest that concomitant use of rilonacept during the first several months of allopurinol therapy may help avoid the acute gout flares that make it difficult for patients to maintain urate-lowering therapy," according to Dr. Mitha. Currently, standard practice includes the use of colchicine or anti-inflammatory drugs to reduce the risk of flares associated with early allopurinol, but the gastrointestinal side effects associated with colchicine in particular can be prohibitive, he said.
Because rilonacept is "very expensive" compared with standard treatment for acute gout flares, studies looking at the relative efficacy of the various treatment options are warranted before the drug should be widely used for this indication, Dr. Mitha stressed.
Dr. Mitha and his coinvestigators disclosed receiving grant/research support from Regeneron Pharmaceuticals, which manufactures rilonacept.
LONDON – Prophylactic treatment with the potent interleukin-1 inhibitor rilonacept significantly reduced the incidence of acute gout flares triggered by the initiation of urate-lowering therapy, according to data from a global phase III study reported at the annual European Congress of Rheumatology.
Patients in the 16-week trial who were randomized to receive weekly subcutaneous injections of either 80 mg or 160 mg of rilonacept (Acralyst) at the outset of standard uric acid–reducing treatment with allopurinol had significantly fewer gout flares and significantly fewer days per flare than did patients randomized to placebo, said principal investigator Dr. Essack Mitha of Newtown Clinical Research in Johannesburg, South Africa.
Further, treatment with the fusion protein, which interrupts the inflammatory cascade by attaching to and neutralizing interleukin-1, demonstrated acceptable safety and tolerability, he said.
The findings are consistent with those of a sister phase III trial in North America reported at the 2010 annual meeting of the American College of Rheumatology, he said.
The phase III, double-blind Preventive Study Against Urate-Lowering Drug-Induced Gout Exacerbations (PRE-SURGE 2) was conducted in South Africa, Germany, and Asia, and included 248 patients with gout, serum uric acid levels of 7.5 mg/dL or higher, and a history of at least two gout flares in the prior year. All of the patients were initiated on 300 mg of allopurinol daily (except those with documented renal dysfunction, who were initiated on a lower dose), and subsequently titrated to achieve target urate levels of less than 6 mg/dL, Dr. Mitha stated.
After the initial allopurinol dose, which was continued for 20 weeks, including a 4-week safety follow-up period, patients were randomized to receive 16 weekly subcutaneous injections of placebo (82 patients), 80 mg of rilonacept with a double dosing on day 1 (82 patients), or 160 mg of rilonacept with a double dosing on day 1 (84 patients). During the study, nonsteroidal anti-inflammatory drugs and oral steroids were allowed for the treatment but not for prevention of gout flares, said Dr. Mitha.
"The primary end point was the mean number of gout flares per patient through week 16. The secondary end points were the proportion of patients experiencing two or more gout flares during this period and the number of flare-days per patient," he said, adding that safety and tolerability were also assessed.
At baseline, the characteristics of the predominantly male (93%) study population were similar across all three groups, with a mean age of 51 years, a mean serum uric acid level of 9.4 mg/dL, a mean of seven gout flares in the prior year, and a mean gout flare duration of 3.8 days. A similar number of patients in the placebo and rilonacept groups completed the treatment period, Dr. Mitha reported.
With respect to the primary end point, the mean number of gout flares per patient was 101 in the placebo group, 29 in the 80-mg rilonacept group, and 28 in the 160-mg rilonacept group, which represent a significant reduction in gout flares relative to placebo, said Dr. Mitha.
"Compared with placebo, the proportion of patients who experienced more than one gout flare through week 16 was reduced by 54% in the 80-mg group and 63% in the 160-mg group," he said. The respective reductions relative to placebo in the proportion of patients experiencing two or more flares were 74% and 82%. "The mean number of gout flare days per patient was also significantly lower in the rilonacept subjects, at 4.3 and 1.9 for the 80-mg and 160-mg groups, respectively, compared with 11.2 for placebo," and significantly fewer patients in the treatment arms had flares lasting 5 days or longer, he said.
In terms of adverse events, the overall incidence was similar across the groups, and although there were more injection-site reactions in the rilonacept groups, "the reactions were generally mild, and none of the patients withdrew for that reason," Dr. Mitha said. Three patients did withdraw from the higher-dose rilonacept group for other reasons – one each for neutropenia, gout flare, and gastric cancer – "but there were no deaths and no serious adverse events related to the product," he stressed.
Together with the results of the North American PRE-SURGE 1 trial, the findings of this study are an important step in the clinical development program for rilonacept, which the U.S. Food and Drug Administration approved in February 2008 for the treatment of cryopyrin-associated periodic syndromes and Muckle-Wells syndrome in adults and children older than 12 years.
"Our results suggest that concomitant use of rilonacept during the first several months of allopurinol therapy may help avoid the acute gout flares that make it difficult for patients to maintain urate-lowering therapy," according to Dr. Mitha. Currently, standard practice includes the use of colchicine or anti-inflammatory drugs to reduce the risk of flares associated with early allopurinol, but the gastrointestinal side effects associated with colchicine in particular can be prohibitive, he said.
Because rilonacept is "very expensive" compared with standard treatment for acute gout flares, studies looking at the relative efficacy of the various treatment options are warranted before the drug should be widely used for this indication, Dr. Mitha stressed.
Dr. Mitha and his coinvestigators disclosed receiving grant/research support from Regeneron Pharmaceuticals, which manufactures rilonacept.
LONDON – Prophylactic treatment with the potent interleukin-1 inhibitor rilonacept significantly reduced the incidence of acute gout flares triggered by the initiation of urate-lowering therapy, according to data from a global phase III study reported at the annual European Congress of Rheumatology.
Patients in the 16-week trial who were randomized to receive weekly subcutaneous injections of either 80 mg or 160 mg of rilonacept (Acralyst) at the outset of standard uric acid–reducing treatment with allopurinol had significantly fewer gout flares and significantly fewer days per flare than did patients randomized to placebo, said principal investigator Dr. Essack Mitha of Newtown Clinical Research in Johannesburg, South Africa.
Further, treatment with the fusion protein, which interrupts the inflammatory cascade by attaching to and neutralizing interleukin-1, demonstrated acceptable safety and tolerability, he said.
The findings are consistent with those of a sister phase III trial in North America reported at the 2010 annual meeting of the American College of Rheumatology, he said.
The phase III, double-blind Preventive Study Against Urate-Lowering Drug-Induced Gout Exacerbations (PRE-SURGE 2) was conducted in South Africa, Germany, and Asia, and included 248 patients with gout, serum uric acid levels of 7.5 mg/dL or higher, and a history of at least two gout flares in the prior year. All of the patients were initiated on 300 mg of allopurinol daily (except those with documented renal dysfunction, who were initiated on a lower dose), and subsequently titrated to achieve target urate levels of less than 6 mg/dL, Dr. Mitha stated.
After the initial allopurinol dose, which was continued for 20 weeks, including a 4-week safety follow-up period, patients were randomized to receive 16 weekly subcutaneous injections of placebo (82 patients), 80 mg of rilonacept with a double dosing on day 1 (82 patients), or 160 mg of rilonacept with a double dosing on day 1 (84 patients). During the study, nonsteroidal anti-inflammatory drugs and oral steroids were allowed for the treatment but not for prevention of gout flares, said Dr. Mitha.
"The primary end point was the mean number of gout flares per patient through week 16. The secondary end points were the proportion of patients experiencing two or more gout flares during this period and the number of flare-days per patient," he said, adding that safety and tolerability were also assessed.
At baseline, the characteristics of the predominantly male (93%) study population were similar across all three groups, with a mean age of 51 years, a mean serum uric acid level of 9.4 mg/dL, a mean of seven gout flares in the prior year, and a mean gout flare duration of 3.8 days. A similar number of patients in the placebo and rilonacept groups completed the treatment period, Dr. Mitha reported.
With respect to the primary end point, the mean number of gout flares per patient was 101 in the placebo group, 29 in the 80-mg rilonacept group, and 28 in the 160-mg rilonacept group, which represent a significant reduction in gout flares relative to placebo, said Dr. Mitha.
"Compared with placebo, the proportion of patients who experienced more than one gout flare through week 16 was reduced by 54% in the 80-mg group and 63% in the 160-mg group," he said. The respective reductions relative to placebo in the proportion of patients experiencing two or more flares were 74% and 82%. "The mean number of gout flare days per patient was also significantly lower in the rilonacept subjects, at 4.3 and 1.9 for the 80-mg and 160-mg groups, respectively, compared with 11.2 for placebo," and significantly fewer patients in the treatment arms had flares lasting 5 days or longer, he said.
In terms of adverse events, the overall incidence was similar across the groups, and although there were more injection-site reactions in the rilonacept groups, "the reactions were generally mild, and none of the patients withdrew for that reason," Dr. Mitha said. Three patients did withdraw from the higher-dose rilonacept group for other reasons – one each for neutropenia, gout flare, and gastric cancer – "but there were no deaths and no serious adverse events related to the product," he stressed.
Together with the results of the North American PRE-SURGE 1 trial, the findings of this study are an important step in the clinical development program for rilonacept, which the U.S. Food and Drug Administration approved in February 2008 for the treatment of cryopyrin-associated periodic syndromes and Muckle-Wells syndrome in adults and children older than 12 years.
"Our results suggest that concomitant use of rilonacept during the first several months of allopurinol therapy may help avoid the acute gout flares that make it difficult for patients to maintain urate-lowering therapy," according to Dr. Mitha. Currently, standard practice includes the use of colchicine or anti-inflammatory drugs to reduce the risk of flares associated with early allopurinol, but the gastrointestinal side effects associated with colchicine in particular can be prohibitive, he said.
Because rilonacept is "very expensive" compared with standard treatment for acute gout flares, studies looking at the relative efficacy of the various treatment options are warranted before the drug should be widely used for this indication, Dr. Mitha stressed.
Dr. Mitha and his coinvestigators disclosed receiving grant/research support from Regeneron Pharmaceuticals, which manufactures rilonacept.
FROM THE ANNUAL EUROPEAN CONGRESS OF RHEUMATOLOGY
Major Finding: The interleukin-1 inhibitor rilonacept reduced the rate of acute gout flares through 16 weeks of treatment by 54% in patients receiving an 80-mg injection and 63% in patients getting 160 mg.
Data Source: A 16-week, phase III, double-blind, randomized trial evaluating the impact of weekly subcutaneous injections of rilonacept on gout flares relative to placebo in 248 patients being treated with allopurinol.
Disclosures: Dr. Mitha and his coinvestigators disclosed receiving grant/research support from Regeneron Pharmaceuticals, which manufactures rilonacept.
Statin Reverses Tofacitinib-Induced Lipid Changes in RA
LONDON – Statin therapy can reverse one of the most important side effects observed in clinical trials of the experimental oral biologic tofacitinib in rheumatoid arthritis, a study has shown.
Concomitant treatment with atorvastatin significantly lessened dyslipidemia observed in a cohort of rheumatoid arthritis patients taking tofacitinib in a phase II trial.
Of 111 rheumatoid arthritis patients enrolled in the study, tofacitinib-treated patients who took atorvastatin (Lipitor) following an open-label lead-in period had a 35% reduction in mean low-density lipoprotein cholesterol (LDL-C) compared with a 5.8% increase observed in tofacitinib-treated patients randomized to concomitant placebo. Those who took atorvastatin had improvements in other lipid measures as well, reported Dr. Iain McInnes of the University of Glasgow (Scotland).
Treatment with tofacitinib, an oral Janus kinase (JAK) inhibitor being investigated as a targeted immunomodulator, has been associated with increases in serum lipids, including LDL and HDL cholesterol and triglycerides in phase II and III rheumatoid arthritis trials, said Dr. McInnes. The same effect is seen with other JAK inhibitors. Certain proinflammatory cytokines have been shown to have an effect on serum lipid levels. Considering the synergy between inflammation and lipid metabolism, "it should be no surprise at all that an agent that modifies inflammation can also cause metabolic changes," he said at the annual European Congress of Rheumatology.
To evaluate whether use of a lipid-lowering drug could safely and effectively modulate lipid increases associated with tofacitinib treatment, Dr. McInnes and his colleagues evaluated the lipid levels of study patients who completed 6 weeks of 10-mg tofacitinib twice daily and were subsequently randomized to an additional 6 weeks of treatment with concomitant atorvastatin or placebo.
From baseline to week 6 of tofacitinib therapy, the average increases for the predominantly female study group (mean age, 52 years) were 185-230 mg/dL for total cholesterol; 109-126 mg/dL for LDL-C; 51-67 mg/dL for high-density lipoprotein cholesterol (HDL-C); 136-165 mg/dL for apolipoprotein A-1; 87-97 mg/dL for apolipoprotein B; and 100-109 mg/dL for triglycerides, Dr. McInnes reported. By week 12, total cholesterol, LDL-C, apolipoprotein B, and triglycerides were significantly decreased in the atorvastatin patients relative to placebo, "to levels below those observed at baseline," he said, while the HDL-C levels increased similarly in both the placebo and atorvastatin groups from week 6 to week 12.
With respect to clinical responses, at week 6, a minimum 20% improvement in American College of Rheumatology criteria (ACR20) was seen in 76% of the study population. "By week 12, 82.6% of the atorvastatin group exhibited an ACR20 response, compared with 65.2% of the placebo group, and 67.4% of the atorvastatin group vs. 45.7% exhibited a minimum 50% improvement in ACR criteria [ACR50)," said Dr. McInnes, who noted that, although the differences in clinical response between the atorvastatin and placebo groups were not statistically significant, the trend toward additional improvements are notable and warrant further study.
In safety analyses, the investigators observed a safety profile similar to that reported in other tofacitinib trials in rheumatoid arthritis, said Dr. McInnes. Specifically, treatment-related adverse events were experienced by 23.4% of the patients during the first 6 weeks of the study, and by 10% of the atorvastatin group and 17% of the placebo group from week 6 to week 12, said Dr. McInnes. Serious adverse events, including pneumonia, occurred in 1.8% of the patients during the open-label phase of the study, he said, noting that none of the atorvastatin patients and 2.1% of the placebo patients experienced serious adverse events between weeks 6 and 12.
"The findings of this study are important in that they demonstrate that any changes in lipids are reversible by addition of a statin," Dr. McInnes said in an interview. "It’s too early to determine how statins and tofacitinib will be used in standard of care. More data are required at this stage."
Dr. Joel Kremer agreed. The chief of medicine at Albany Medical College in New York, Dr. Kremer was the lead investigator of a phase III trial that he reported at the meeting. Data from the phase III trial demonstrated the efficacy of tofacitinib in rheumatoid arthritis patients who failed to respond to treatment with other disease-modifying antirheumatic drugs.
In an interview, Dr. Kremer noted that it’s uncertain whether concurrent lipid-lowering therapy will be considered routine standard of care with tofacitinib in rheumatoid arthritis patients, "but it probably will become quite common, as it is becoming common with Actemra [tocilizumab]."
Dr. McInnes and Dr. Kremer disclosed receiving grant and research support from and serving as consultants for Pfizer.
LONDON – Statin therapy can reverse one of the most important side effects observed in clinical trials of the experimental oral biologic tofacitinib in rheumatoid arthritis, a study has shown.
Concomitant treatment with atorvastatin significantly lessened dyslipidemia observed in a cohort of rheumatoid arthritis patients taking tofacitinib in a phase II trial.
Of 111 rheumatoid arthritis patients enrolled in the study, tofacitinib-treated patients who took atorvastatin (Lipitor) following an open-label lead-in period had a 35% reduction in mean low-density lipoprotein cholesterol (LDL-C) compared with a 5.8% increase observed in tofacitinib-treated patients randomized to concomitant placebo. Those who took atorvastatin had improvements in other lipid measures as well, reported Dr. Iain McInnes of the University of Glasgow (Scotland).
Treatment with tofacitinib, an oral Janus kinase (JAK) inhibitor being investigated as a targeted immunomodulator, has been associated with increases in serum lipids, including LDL and HDL cholesterol and triglycerides in phase II and III rheumatoid arthritis trials, said Dr. McInnes. The same effect is seen with other JAK inhibitors. Certain proinflammatory cytokines have been shown to have an effect on serum lipid levels. Considering the synergy between inflammation and lipid metabolism, "it should be no surprise at all that an agent that modifies inflammation can also cause metabolic changes," he said at the annual European Congress of Rheumatology.
To evaluate whether use of a lipid-lowering drug could safely and effectively modulate lipid increases associated with tofacitinib treatment, Dr. McInnes and his colleagues evaluated the lipid levels of study patients who completed 6 weeks of 10-mg tofacitinib twice daily and were subsequently randomized to an additional 6 weeks of treatment with concomitant atorvastatin or placebo.
From baseline to week 6 of tofacitinib therapy, the average increases for the predominantly female study group (mean age, 52 years) were 185-230 mg/dL for total cholesterol; 109-126 mg/dL for LDL-C; 51-67 mg/dL for high-density lipoprotein cholesterol (HDL-C); 136-165 mg/dL for apolipoprotein A-1; 87-97 mg/dL for apolipoprotein B; and 100-109 mg/dL for triglycerides, Dr. McInnes reported. By week 12, total cholesterol, LDL-C, apolipoprotein B, and triglycerides were significantly decreased in the atorvastatin patients relative to placebo, "to levels below those observed at baseline," he said, while the HDL-C levels increased similarly in both the placebo and atorvastatin groups from week 6 to week 12.
With respect to clinical responses, at week 6, a minimum 20% improvement in American College of Rheumatology criteria (ACR20) was seen in 76% of the study population. "By week 12, 82.6% of the atorvastatin group exhibited an ACR20 response, compared with 65.2% of the placebo group, and 67.4% of the atorvastatin group vs. 45.7% exhibited a minimum 50% improvement in ACR criteria [ACR50)," said Dr. McInnes, who noted that, although the differences in clinical response between the atorvastatin and placebo groups were not statistically significant, the trend toward additional improvements are notable and warrant further study.
In safety analyses, the investigators observed a safety profile similar to that reported in other tofacitinib trials in rheumatoid arthritis, said Dr. McInnes. Specifically, treatment-related adverse events were experienced by 23.4% of the patients during the first 6 weeks of the study, and by 10% of the atorvastatin group and 17% of the placebo group from week 6 to week 12, said Dr. McInnes. Serious adverse events, including pneumonia, occurred in 1.8% of the patients during the open-label phase of the study, he said, noting that none of the atorvastatin patients and 2.1% of the placebo patients experienced serious adverse events between weeks 6 and 12.
"The findings of this study are important in that they demonstrate that any changes in lipids are reversible by addition of a statin," Dr. McInnes said in an interview. "It’s too early to determine how statins and tofacitinib will be used in standard of care. More data are required at this stage."
Dr. Joel Kremer agreed. The chief of medicine at Albany Medical College in New York, Dr. Kremer was the lead investigator of a phase III trial that he reported at the meeting. Data from the phase III trial demonstrated the efficacy of tofacitinib in rheumatoid arthritis patients who failed to respond to treatment with other disease-modifying antirheumatic drugs.
In an interview, Dr. Kremer noted that it’s uncertain whether concurrent lipid-lowering therapy will be considered routine standard of care with tofacitinib in rheumatoid arthritis patients, "but it probably will become quite common, as it is becoming common with Actemra [tocilizumab]."
Dr. McInnes and Dr. Kremer disclosed receiving grant and research support from and serving as consultants for Pfizer.
LONDON – Statin therapy can reverse one of the most important side effects observed in clinical trials of the experimental oral biologic tofacitinib in rheumatoid arthritis, a study has shown.
Concomitant treatment with atorvastatin significantly lessened dyslipidemia observed in a cohort of rheumatoid arthritis patients taking tofacitinib in a phase II trial.
Of 111 rheumatoid arthritis patients enrolled in the study, tofacitinib-treated patients who took atorvastatin (Lipitor) following an open-label lead-in period had a 35% reduction in mean low-density lipoprotein cholesterol (LDL-C) compared with a 5.8% increase observed in tofacitinib-treated patients randomized to concomitant placebo. Those who took atorvastatin had improvements in other lipid measures as well, reported Dr. Iain McInnes of the University of Glasgow (Scotland).
Treatment with tofacitinib, an oral Janus kinase (JAK) inhibitor being investigated as a targeted immunomodulator, has been associated with increases in serum lipids, including LDL and HDL cholesterol and triglycerides in phase II and III rheumatoid arthritis trials, said Dr. McInnes. The same effect is seen with other JAK inhibitors. Certain proinflammatory cytokines have been shown to have an effect on serum lipid levels. Considering the synergy between inflammation and lipid metabolism, "it should be no surprise at all that an agent that modifies inflammation can also cause metabolic changes," he said at the annual European Congress of Rheumatology.
To evaluate whether use of a lipid-lowering drug could safely and effectively modulate lipid increases associated with tofacitinib treatment, Dr. McInnes and his colleagues evaluated the lipid levels of study patients who completed 6 weeks of 10-mg tofacitinib twice daily and were subsequently randomized to an additional 6 weeks of treatment with concomitant atorvastatin or placebo.
From baseline to week 6 of tofacitinib therapy, the average increases for the predominantly female study group (mean age, 52 years) were 185-230 mg/dL for total cholesterol; 109-126 mg/dL for LDL-C; 51-67 mg/dL for high-density lipoprotein cholesterol (HDL-C); 136-165 mg/dL for apolipoprotein A-1; 87-97 mg/dL for apolipoprotein B; and 100-109 mg/dL for triglycerides, Dr. McInnes reported. By week 12, total cholesterol, LDL-C, apolipoprotein B, and triglycerides were significantly decreased in the atorvastatin patients relative to placebo, "to levels below those observed at baseline," he said, while the HDL-C levels increased similarly in both the placebo and atorvastatin groups from week 6 to week 12.
With respect to clinical responses, at week 6, a minimum 20% improvement in American College of Rheumatology criteria (ACR20) was seen in 76% of the study population. "By week 12, 82.6% of the atorvastatin group exhibited an ACR20 response, compared with 65.2% of the placebo group, and 67.4% of the atorvastatin group vs. 45.7% exhibited a minimum 50% improvement in ACR criteria [ACR50)," said Dr. McInnes, who noted that, although the differences in clinical response between the atorvastatin and placebo groups were not statistically significant, the trend toward additional improvements are notable and warrant further study.
In safety analyses, the investigators observed a safety profile similar to that reported in other tofacitinib trials in rheumatoid arthritis, said Dr. McInnes. Specifically, treatment-related adverse events were experienced by 23.4% of the patients during the first 6 weeks of the study, and by 10% of the atorvastatin group and 17% of the placebo group from week 6 to week 12, said Dr. McInnes. Serious adverse events, including pneumonia, occurred in 1.8% of the patients during the open-label phase of the study, he said, noting that none of the atorvastatin patients and 2.1% of the placebo patients experienced serious adverse events between weeks 6 and 12.
"The findings of this study are important in that they demonstrate that any changes in lipids are reversible by addition of a statin," Dr. McInnes said in an interview. "It’s too early to determine how statins and tofacitinib will be used in standard of care. More data are required at this stage."
Dr. Joel Kremer agreed. The chief of medicine at Albany Medical College in New York, Dr. Kremer was the lead investigator of a phase III trial that he reported at the meeting. Data from the phase III trial demonstrated the efficacy of tofacitinib in rheumatoid arthritis patients who failed to respond to treatment with other disease-modifying antirheumatic drugs.
In an interview, Dr. Kremer noted that it’s uncertain whether concurrent lipid-lowering therapy will be considered routine standard of care with tofacitinib in rheumatoid arthritis patients, "but it probably will become quite common, as it is becoming common with Actemra [tocilizumab]."
Dr. McInnes and Dr. Kremer disclosed receiving grant and research support from and serving as consultants for Pfizer.
FROM THE ANNUAL EUROPEAN CONGRESS OF RHEUMATOLOGY
Major Finding: The lipid-lowering drug atorvastatin was associated with a 35% reduction in mean low-density lipoprotein cholesterol relative to placebo in rheumatoid arthritis patients taking the experimental oral JAK inhibitor tofacitinib.
Data Source: An open-label tofacitinib, double-blind atorvastatin study of lipid metabolism in 111 rheumatoid arthritis patients.
Disclosures: Dr. McInnes and Dr. Kremer disclosed receiving grant and research support from and serving as consultants for Pfizer.
Statin Reverses Tofacitinib-Induced Lipid Changes in RA
LONDON – Statin therapy can reverse one of the most important side effects observed in clinical trials of the experimental oral biologic tofacitinib in rheumatoid arthritis, a study has shown.
Concomitant treatment with atorvastatin significantly lessened dyslipidemia observed in a cohort of rheumatoid arthritis patients taking tofacitinib in a phase II trial.
Of 111 rheumatoid arthritis patients enrolled in the study, tofacitinib-treated patients who took atorvastatin (Lipitor) following an open-label lead-in period had a 35% reduction in mean low-density lipoprotein cholesterol (LDL-C) compared with a 5.8% increase observed in tofacitinib-treated patients randomized to concomitant placebo. Those who took atorvastatin had improvements in other lipid measures as well, reported Dr. Iain McInnes of the University of Glasgow (Scotland).
Treatment with tofacitinib, an oral Janus kinase (JAK) inhibitor being investigated as a targeted immunomodulator, has been associated with increases in serum lipids, including LDL and HDL cholesterol and triglycerides in phase II and III rheumatoid arthritis trials, said Dr. McInnes. The same effect is seen with other JAK inhibitors. Certain proinflammatory cytokines have been shown to have an effect on serum lipid levels. Considering the synergy between inflammation and lipid metabolism, "it should be no surprise at all that an agent that modifies inflammation can also cause metabolic changes," he said at the annual European Congress of Rheumatology.
To evaluate whether use of a lipid-lowering drug could safely and effectively modulate lipid increases associated with tofacitinib treatment, Dr. McInnes and his colleagues evaluated the lipid levels of study patients who completed 6 weeks of 10-mg tofacitinib twice daily and were subsequently randomized to an additional 6 weeks of treatment with concomitant atorvastatin or placebo.
From baseline to week 6 of tofacitinib therapy, the average increases for the predominantly female study group (mean age, 52 years) were 185-230 mg/dL for total cholesterol; 109-126 mg/dL for LDL-C; 51-67 mg/dL for high-density lipoprotein cholesterol (HDL-C); 136-165 mg/dL for apolipoprotein A-1; 87-97 mg/dL for apolipoprotein B; and 100-109 mg/dL for triglycerides, Dr. McInnes reported. By week 12, total cholesterol, LDL-C, apolipoprotein B, and triglycerides were significantly decreased in the atorvastatin patients relative to placebo, "to levels below those observed at baseline," he said, while the HDL-C levels increased similarly in both the placebo and atorvastatin groups from week 6 to week 12.
With respect to clinical responses, at week 6, a minimum 20% improvement in American College of Rheumatology criteria (ACR20) was seen in 76% of the study population. "By week 12, 82.6% of the atorvastatin group exhibited an ACR20 response, compared with 65.2% of the placebo group, and 67.4% of the atorvastatin group vs. 45.7% exhibited a minimum 50% improvement in ACR criteria [ACR50)," said Dr. McInnes, who noted that, although the differences in clinical response between the atorvastatin and placebo groups were not statistically significant, the trend toward additional improvements are notable and warrant further study.
In safety analyses, the investigators observed a safety profile similar to that reported in other tofacitinib trials in rheumatoid arthritis, said Dr. McInnes. Specifically, treatment-related adverse events were experienced by 23.4% of the patients during the first 6 weeks of the study, and by 10% of the atorvastatin group and 17% of the placebo group from week 6 to week 12, said Dr. McInnes. Serious adverse events, including pneumonia, occurred in 1.8% of the patients during the open-label phase of the study, he said, noting that none of the atorvastatin patients and 2.1% of the placebo patients experienced serious adverse events between weeks 6 and 12.
"The findings of this study are important in that they demonstrate that any changes in lipids are reversible by addition of a statin," Dr. McInnes said in an interview. "It’s too early to determine how statins and tofacitinib will be used in standard of care. More data are required at this stage."
Dr. Joel Kremer agreed. The chief of medicine at Albany Medical College in New York, Dr. Kremer was the lead investigator of a phase III trial that he reported at the meeting. Data from the phase III trial demonstrated the efficacy of tofacitinib in rheumatoid arthritis patients who failed to respond to treatment with other disease-modifying antirheumatic drugs.
In an interview, Dr. Kremer noted that it’s uncertain whether concurrent lipid-lowering therapy will be considered routine standard of care with tofacitinib in rheumatoid arthritis patients, "but it probably will become quite common, as it is becoming common with Actemra [tocilizumab]."
Dr. McInnes and Dr. Kremer disclosed receiving grant and research support from and serving as consultants for Pfizer.
LONDON – Statin therapy can reverse one of the most important side effects observed in clinical trials of the experimental oral biologic tofacitinib in rheumatoid arthritis, a study has shown.
Concomitant treatment with atorvastatin significantly lessened dyslipidemia observed in a cohort of rheumatoid arthritis patients taking tofacitinib in a phase II trial.
Of 111 rheumatoid arthritis patients enrolled in the study, tofacitinib-treated patients who took atorvastatin (Lipitor) following an open-label lead-in period had a 35% reduction in mean low-density lipoprotein cholesterol (LDL-C) compared with a 5.8% increase observed in tofacitinib-treated patients randomized to concomitant placebo. Those who took atorvastatin had improvements in other lipid measures as well, reported Dr. Iain McInnes of the University of Glasgow (Scotland).
Treatment with tofacitinib, an oral Janus kinase (JAK) inhibitor being investigated as a targeted immunomodulator, has been associated with increases in serum lipids, including LDL and HDL cholesterol and triglycerides in phase II and III rheumatoid arthritis trials, said Dr. McInnes. The same effect is seen with other JAK inhibitors. Certain proinflammatory cytokines have been shown to have an effect on serum lipid levels. Considering the synergy between inflammation and lipid metabolism, "it should be no surprise at all that an agent that modifies inflammation can also cause metabolic changes," he said at the annual European Congress of Rheumatology.
To evaluate whether use of a lipid-lowering drug could safely and effectively modulate lipid increases associated with tofacitinib treatment, Dr. McInnes and his colleagues evaluated the lipid levels of study patients who completed 6 weeks of 10-mg tofacitinib twice daily and were subsequently randomized to an additional 6 weeks of treatment with concomitant atorvastatin or placebo.
From baseline to week 6 of tofacitinib therapy, the average increases for the predominantly female study group (mean age, 52 years) were 185-230 mg/dL for total cholesterol; 109-126 mg/dL for LDL-C; 51-67 mg/dL for high-density lipoprotein cholesterol (HDL-C); 136-165 mg/dL for apolipoprotein A-1; 87-97 mg/dL for apolipoprotein B; and 100-109 mg/dL for triglycerides, Dr. McInnes reported. By week 12, total cholesterol, LDL-C, apolipoprotein B, and triglycerides were significantly decreased in the atorvastatin patients relative to placebo, "to levels below those observed at baseline," he said, while the HDL-C levels increased similarly in both the placebo and atorvastatin groups from week 6 to week 12.
With respect to clinical responses, at week 6, a minimum 20% improvement in American College of Rheumatology criteria (ACR20) was seen in 76% of the study population. "By week 12, 82.6% of the atorvastatin group exhibited an ACR20 response, compared with 65.2% of the placebo group, and 67.4% of the atorvastatin group vs. 45.7% exhibited a minimum 50% improvement in ACR criteria [ACR50)," said Dr. McInnes, who noted that, although the differences in clinical response between the atorvastatin and placebo groups were not statistically significant, the trend toward additional improvements are notable and warrant further study.
In safety analyses, the investigators observed a safety profile similar to that reported in other tofacitinib trials in rheumatoid arthritis, said Dr. McInnes. Specifically, treatment-related adverse events were experienced by 23.4% of the patients during the first 6 weeks of the study, and by 10% of the atorvastatin group and 17% of the placebo group from week 6 to week 12, said Dr. McInnes. Serious adverse events, including pneumonia, occurred in 1.8% of the patients during the open-label phase of the study, he said, noting that none of the atorvastatin patients and 2.1% of the placebo patients experienced serious adverse events between weeks 6 and 12.
"The findings of this study are important in that they demonstrate that any changes in lipids are reversible by addition of a statin," Dr. McInnes said in an interview. "It’s too early to determine how statins and tofacitinib will be used in standard of care. More data are required at this stage."
Dr. Joel Kremer agreed. The chief of medicine at Albany Medical College in New York, Dr. Kremer was the lead investigator of a phase III trial that he reported at the meeting. Data from the phase III trial demonstrated the efficacy of tofacitinib in rheumatoid arthritis patients who failed to respond to treatment with other disease-modifying antirheumatic drugs.
In an interview, Dr. Kremer noted that it’s uncertain whether concurrent lipid-lowering therapy will be considered routine standard of care with tofacitinib in rheumatoid arthritis patients, "but it probably will become quite common, as it is becoming common with Actemra [tocilizumab]."
Dr. McInnes and Dr. Kremer disclosed receiving grant and research support from and serving as consultants for Pfizer.
LONDON – Statin therapy can reverse one of the most important side effects observed in clinical trials of the experimental oral biologic tofacitinib in rheumatoid arthritis, a study has shown.
Concomitant treatment with atorvastatin significantly lessened dyslipidemia observed in a cohort of rheumatoid arthritis patients taking tofacitinib in a phase II trial.
Of 111 rheumatoid arthritis patients enrolled in the study, tofacitinib-treated patients who took atorvastatin (Lipitor) following an open-label lead-in period had a 35% reduction in mean low-density lipoprotein cholesterol (LDL-C) compared with a 5.8% increase observed in tofacitinib-treated patients randomized to concomitant placebo. Those who took atorvastatin had improvements in other lipid measures as well, reported Dr. Iain McInnes of the University of Glasgow (Scotland).
Treatment with tofacitinib, an oral Janus kinase (JAK) inhibitor being investigated as a targeted immunomodulator, has been associated with increases in serum lipids, including LDL and HDL cholesterol and triglycerides in phase II and III rheumatoid arthritis trials, said Dr. McInnes. The same effect is seen with other JAK inhibitors. Certain proinflammatory cytokines have been shown to have an effect on serum lipid levels. Considering the synergy between inflammation and lipid metabolism, "it should be no surprise at all that an agent that modifies inflammation can also cause metabolic changes," he said at the annual European Congress of Rheumatology.
To evaluate whether use of a lipid-lowering drug could safely and effectively modulate lipid increases associated with tofacitinib treatment, Dr. McInnes and his colleagues evaluated the lipid levels of study patients who completed 6 weeks of 10-mg tofacitinib twice daily and were subsequently randomized to an additional 6 weeks of treatment with concomitant atorvastatin or placebo.
From baseline to week 6 of tofacitinib therapy, the average increases for the predominantly female study group (mean age, 52 years) were 185-230 mg/dL for total cholesterol; 109-126 mg/dL for LDL-C; 51-67 mg/dL for high-density lipoprotein cholesterol (HDL-C); 136-165 mg/dL for apolipoprotein A-1; 87-97 mg/dL for apolipoprotein B; and 100-109 mg/dL for triglycerides, Dr. McInnes reported. By week 12, total cholesterol, LDL-C, apolipoprotein B, and triglycerides were significantly decreased in the atorvastatin patients relative to placebo, "to levels below those observed at baseline," he said, while the HDL-C levels increased similarly in both the placebo and atorvastatin groups from week 6 to week 12.
With respect to clinical responses, at week 6, a minimum 20% improvement in American College of Rheumatology criteria (ACR20) was seen in 76% of the study population. "By week 12, 82.6% of the atorvastatin group exhibited an ACR20 response, compared with 65.2% of the placebo group, and 67.4% of the atorvastatin group vs. 45.7% exhibited a minimum 50% improvement in ACR criteria [ACR50)," said Dr. McInnes, who noted that, although the differences in clinical response between the atorvastatin and placebo groups were not statistically significant, the trend toward additional improvements are notable and warrant further study.
In safety analyses, the investigators observed a safety profile similar to that reported in other tofacitinib trials in rheumatoid arthritis, said Dr. McInnes. Specifically, treatment-related adverse events were experienced by 23.4% of the patients during the first 6 weeks of the study, and by 10% of the atorvastatin group and 17% of the placebo group from week 6 to week 12, said Dr. McInnes. Serious adverse events, including pneumonia, occurred in 1.8% of the patients during the open-label phase of the study, he said, noting that none of the atorvastatin patients and 2.1% of the placebo patients experienced serious adverse events between weeks 6 and 12.
"The findings of this study are important in that they demonstrate that any changes in lipids are reversible by addition of a statin," Dr. McInnes said in an interview. "It’s too early to determine how statins and tofacitinib will be used in standard of care. More data are required at this stage."
Dr. Joel Kremer agreed. The chief of medicine at Albany Medical College in New York, Dr. Kremer was the lead investigator of a phase III trial that he reported at the meeting. Data from the phase III trial demonstrated the efficacy of tofacitinib in rheumatoid arthritis patients who failed to respond to treatment with other disease-modifying antirheumatic drugs.
In an interview, Dr. Kremer noted that it’s uncertain whether concurrent lipid-lowering therapy will be considered routine standard of care with tofacitinib in rheumatoid arthritis patients, "but it probably will become quite common, as it is becoming common with Actemra [tocilizumab]."
Dr. McInnes and Dr. Kremer disclosed receiving grant and research support from and serving as consultants for Pfizer.
FROM THE ANNUAL EUROPEAN CONGRESS OF RHEUMATOLOGY
Major Finding: The lipid-lowering drug atorvastatin was associated with a 35% reduction in mean low-density lipoprotein cholesterol relative to placebo in rheumatoid arthritis patients taking the experimental oral JAK inhibitor tofacitinib.
Data Source: An open-label tofacitinib, double-blind atorvastatin study of lipid metabolism in 111 rheumatoid arthritis patients.
Disclosures: Dr. McInnes and Dr. Kremer disclosed receiving grant and research support from and serving as consultants for Pfizer.
Gout Raises MI Risk in Young, Low Risk
LONDON – Gout is an independent risk factor for acute myocardial infarction, even among younger patients and those without cardiovascular risk factors, according to Dr. Chang-Fu Kuo, who presented a late-breaking report at the Annual European Congress of Rheumatology.
The risk for acute MI was 23% higher among gout patients than the general population, judging from an analysis of a large Taiwanese database. Among individuals aged 20-44 years old and those without additional cardiovascular risk factors, the risk of acute MI was increased by 59% and 76%, respectively, reported Dr. Kuo of Chang Gung Memorial Hospital, Taipei, Taiwan.
To investigate the risk of acute MI associated with gout, Dr. Kuo and colleagues analyzed the 2000 Taiwan National Health Insurance database, which is a representative sampling cohort of the general population. Specifically, the investigators compared rates of first hospital admission for acute MI among gout and nongout patients aged 20 years or older. Of the 704,503 individuals included in the cohort (mean age, 42.73 years), 26,566 were diagnosed and treated for gout in 1996-1999, Dr. Kuo said. Compared with the nongout patients, "the gout patients were significantly older, with a mean age of 55.4 years, and they were significantly more likely to have diabetes and hypertension," he said.
The investigators followed the cohort from January 2000 through December 2008, for a total of 5.6 million patient-years of follow-up. During this period, 3,718 patients were hospitalized for acute MI, including 463 patients with gout. Of these events, 299 were fatal, including 35 in gout patients, Dr. Kuo said. "The incidence of acute [MI] in gout patients was 2.20 per 1,000 patient years and was significantly higher than in nongout patients, which was 0.60," he said.
In the multivariate model adjusted for age, sex, diabetes, hypertension, coronary heart disease, stroke, and end-stage renal disease, the respective hazard ratios for all acute MI and nonfatal acute MI in gout patients were 1.23 and 1.26, Dr. Kuo reported. "In patients without cardiovascular risk factors, the hazard ratio for all acute [MI] was 1.84, and for nonfatal acute [MI] was 1.80," he said, and when assessed by age, the respective hazard ratios for gout patients aged 20-44 years, 45-59 years, and 60 years or older were 1.59, 1.24, and 1.11.
The multivariate model was not adjusted for hyperlipidemia, which has been associated with gout, Dr. Kuo said, acknowledging that elevated lipid levels could play an important role in the increased cardiovascular risks observed in the gout patients.
Although the increased risk of acute MI associated with gout has been previously reported, "the risk in younger patients and those with low risk profiles hasn’t previously been established," Dr. Kuo explained. The finding that gout is an independent risk factor for the occurrence of acute MI – particularly nonfatal acute MI – among young, low-risk patients suggests the need for "vigilant cardiovascular monitoring" of these patients, he stressed.
Dr. Kuo reported having no conflicts of interest to disclose.
LONDON – Gout is an independent risk factor for acute myocardial infarction, even among younger patients and those without cardiovascular risk factors, according to Dr. Chang-Fu Kuo, who presented a late-breaking report at the Annual European Congress of Rheumatology.
The risk for acute MI was 23% higher among gout patients than the general population, judging from an analysis of a large Taiwanese database. Among individuals aged 20-44 years old and those without additional cardiovascular risk factors, the risk of acute MI was increased by 59% and 76%, respectively, reported Dr. Kuo of Chang Gung Memorial Hospital, Taipei, Taiwan.
To investigate the risk of acute MI associated with gout, Dr. Kuo and colleagues analyzed the 2000 Taiwan National Health Insurance database, which is a representative sampling cohort of the general population. Specifically, the investigators compared rates of first hospital admission for acute MI among gout and nongout patients aged 20 years or older. Of the 704,503 individuals included in the cohort (mean age, 42.73 years), 26,566 were diagnosed and treated for gout in 1996-1999, Dr. Kuo said. Compared with the nongout patients, "the gout patients were significantly older, with a mean age of 55.4 years, and they were significantly more likely to have diabetes and hypertension," he said.
The investigators followed the cohort from January 2000 through December 2008, for a total of 5.6 million patient-years of follow-up. During this period, 3,718 patients were hospitalized for acute MI, including 463 patients with gout. Of these events, 299 were fatal, including 35 in gout patients, Dr. Kuo said. "The incidence of acute [MI] in gout patients was 2.20 per 1,000 patient years and was significantly higher than in nongout patients, which was 0.60," he said.
In the multivariate model adjusted for age, sex, diabetes, hypertension, coronary heart disease, stroke, and end-stage renal disease, the respective hazard ratios for all acute MI and nonfatal acute MI in gout patients were 1.23 and 1.26, Dr. Kuo reported. "In patients without cardiovascular risk factors, the hazard ratio for all acute [MI] was 1.84, and for nonfatal acute [MI] was 1.80," he said, and when assessed by age, the respective hazard ratios for gout patients aged 20-44 years, 45-59 years, and 60 years or older were 1.59, 1.24, and 1.11.
The multivariate model was not adjusted for hyperlipidemia, which has been associated with gout, Dr. Kuo said, acknowledging that elevated lipid levels could play an important role in the increased cardiovascular risks observed in the gout patients.
Although the increased risk of acute MI associated with gout has been previously reported, "the risk in younger patients and those with low risk profiles hasn’t previously been established," Dr. Kuo explained. The finding that gout is an independent risk factor for the occurrence of acute MI – particularly nonfatal acute MI – among young, low-risk patients suggests the need for "vigilant cardiovascular monitoring" of these patients, he stressed.
Dr. Kuo reported having no conflicts of interest to disclose.
LONDON – Gout is an independent risk factor for acute myocardial infarction, even among younger patients and those without cardiovascular risk factors, according to Dr. Chang-Fu Kuo, who presented a late-breaking report at the Annual European Congress of Rheumatology.
The risk for acute MI was 23% higher among gout patients than the general population, judging from an analysis of a large Taiwanese database. Among individuals aged 20-44 years old and those without additional cardiovascular risk factors, the risk of acute MI was increased by 59% and 76%, respectively, reported Dr. Kuo of Chang Gung Memorial Hospital, Taipei, Taiwan.
To investigate the risk of acute MI associated with gout, Dr. Kuo and colleagues analyzed the 2000 Taiwan National Health Insurance database, which is a representative sampling cohort of the general population. Specifically, the investigators compared rates of first hospital admission for acute MI among gout and nongout patients aged 20 years or older. Of the 704,503 individuals included in the cohort (mean age, 42.73 years), 26,566 were diagnosed and treated for gout in 1996-1999, Dr. Kuo said. Compared with the nongout patients, "the gout patients were significantly older, with a mean age of 55.4 years, and they were significantly more likely to have diabetes and hypertension," he said.
The investigators followed the cohort from January 2000 through December 2008, for a total of 5.6 million patient-years of follow-up. During this period, 3,718 patients were hospitalized for acute MI, including 463 patients with gout. Of these events, 299 were fatal, including 35 in gout patients, Dr. Kuo said. "The incidence of acute [MI] in gout patients was 2.20 per 1,000 patient years and was significantly higher than in nongout patients, which was 0.60," he said.
In the multivariate model adjusted for age, sex, diabetes, hypertension, coronary heart disease, stroke, and end-stage renal disease, the respective hazard ratios for all acute MI and nonfatal acute MI in gout patients were 1.23 and 1.26, Dr. Kuo reported. "In patients without cardiovascular risk factors, the hazard ratio for all acute [MI] was 1.84, and for nonfatal acute [MI] was 1.80," he said, and when assessed by age, the respective hazard ratios for gout patients aged 20-44 years, 45-59 years, and 60 years or older were 1.59, 1.24, and 1.11.
The multivariate model was not adjusted for hyperlipidemia, which has been associated with gout, Dr. Kuo said, acknowledging that elevated lipid levels could play an important role in the increased cardiovascular risks observed in the gout patients.
Although the increased risk of acute MI associated with gout has been previously reported, "the risk in younger patients and those with low risk profiles hasn’t previously been established," Dr. Kuo explained. The finding that gout is an independent risk factor for the occurrence of acute MI – particularly nonfatal acute MI – among young, low-risk patients suggests the need for "vigilant cardiovascular monitoring" of these patients, he stressed.
Dr. Kuo reported having no conflicts of interest to disclose.
FROM THE ANNUAL EUROPEAN CONGRESS OF RHEUMATOLOGY
Major Finding: The incidence of acute MI was increased by 76% in people aged 20-44 years who had no other cardiac risk factors except gout, compared with the general population.
Data Source: A representative sampling cohort representing 1 million randomly selected subjects from the general population of Taiwan.
Disclosures: Dr. Kuo reported having no conflicts to disclose.
Gout Raises MI Risk in Young, Low Risk
LONDON – Gout is an independent risk factor for acute myocardial infarction, even among younger patients and those without cardiovascular risk factors, according to Dr. Chang-Fu Kuo, who presented a late-breaking report at the Annual European Congress of Rheumatology.
The risk for acute MI was 23% higher among gout patients than the general population, judging from an analysis of a large Taiwanese database. Among individuals aged 20-44 years old and those without additional cardiovascular risk factors, the risk of acute MI was increased by 59% and 76%, respectively, reported Dr. Kuo of Chang Gung Memorial Hospital, Taipei, Taiwan.
To investigate the risk of acute MI associated with gout, Dr. Kuo and colleagues analyzed the 2000 Taiwan National Health Insurance database, which is a representative sampling cohort of the general population. Specifically, the investigators compared rates of first hospital admission for acute MI among gout and nongout patients aged 20 years or older. Of the 704,503 individuals included in the cohort (mean age, 42.73 years), 26,566 were diagnosed and treated for gout in 1996-1999, Dr. Kuo said. Compared with the nongout patients, "the gout patients were significantly older, with a mean age of 55.4 years, and they were significantly more likely to have diabetes and hypertension," he said.
The investigators followed the cohort from January 2000 through December 2008, for a total of 5.6 million patient-years of follow-up. During this period, 3,718 patients were hospitalized for acute MI, including 463 patients with gout. Of these events, 299 were fatal, including 35 in gout patients, Dr. Kuo said. "The incidence of acute [MI] in gout patients was 2.20 per 1,000 patient years and was significantly higher than in nongout patients, which was 0.60," he said.
In the multivariate model adjusted for age, sex, diabetes, hypertension, coronary heart disease, stroke, and end-stage renal disease, the respective hazard ratios for all acute MI and nonfatal acute MI in gout patients were 1.23 and 1.26, Dr. Kuo reported. "In patients without cardiovascular risk factors, the hazard ratio for all acute [MI] was 1.84, and for nonfatal acute [MI] was 1.80," he said, and when assessed by age, the respective hazard ratios for gout patients aged 20-44 years, 45-59 years, and 60 years or older were 1.59, 1.24, and 1.11.
The multivariate model was not adjusted for hyperlipidemia, which has been associated with gout, Dr. Kuo said, acknowledging that elevated lipid levels could play an important role in the increased cardiovascular risks observed in the gout patients.
Although the increased risk of acute MI associated with gout has been previously reported, "the risk in younger patients and those with low risk profiles hasn’t previously been established," Dr. Kuo explained. The finding that gout is an independent risk factor for the occurrence of acute MI – particularly nonfatal acute MI – among young, low-risk patients suggests the need for "vigilant cardiovascular monitoring" of these patients, he stressed.
Dr. Kuo reported having no conflicts of interest to disclose.
LONDON – Gout is an independent risk factor for acute myocardial infarction, even among younger patients and those without cardiovascular risk factors, according to Dr. Chang-Fu Kuo, who presented a late-breaking report at the Annual European Congress of Rheumatology.
The risk for acute MI was 23% higher among gout patients than the general population, judging from an analysis of a large Taiwanese database. Among individuals aged 20-44 years old and those without additional cardiovascular risk factors, the risk of acute MI was increased by 59% and 76%, respectively, reported Dr. Kuo of Chang Gung Memorial Hospital, Taipei, Taiwan.
To investigate the risk of acute MI associated with gout, Dr. Kuo and colleagues analyzed the 2000 Taiwan National Health Insurance database, which is a representative sampling cohort of the general population. Specifically, the investigators compared rates of first hospital admission for acute MI among gout and nongout patients aged 20 years or older. Of the 704,503 individuals included in the cohort (mean age, 42.73 years), 26,566 were diagnosed and treated for gout in 1996-1999, Dr. Kuo said. Compared with the nongout patients, "the gout patients were significantly older, with a mean age of 55.4 years, and they were significantly more likely to have diabetes and hypertension," he said.
The investigators followed the cohort from January 2000 through December 2008, for a total of 5.6 million patient-years of follow-up. During this period, 3,718 patients were hospitalized for acute MI, including 463 patients with gout. Of these events, 299 were fatal, including 35 in gout patients, Dr. Kuo said. "The incidence of acute [MI] in gout patients was 2.20 per 1,000 patient years and was significantly higher than in nongout patients, which was 0.60," he said.
In the multivariate model adjusted for age, sex, diabetes, hypertension, coronary heart disease, stroke, and end-stage renal disease, the respective hazard ratios for all acute MI and nonfatal acute MI in gout patients were 1.23 and 1.26, Dr. Kuo reported. "In patients without cardiovascular risk factors, the hazard ratio for all acute [MI] was 1.84, and for nonfatal acute [MI] was 1.80," he said, and when assessed by age, the respective hazard ratios for gout patients aged 20-44 years, 45-59 years, and 60 years or older were 1.59, 1.24, and 1.11.
The multivariate model was not adjusted for hyperlipidemia, which has been associated with gout, Dr. Kuo said, acknowledging that elevated lipid levels could play an important role in the increased cardiovascular risks observed in the gout patients.
Although the increased risk of acute MI associated with gout has been previously reported, "the risk in younger patients and those with low risk profiles hasn’t previously been established," Dr. Kuo explained. The finding that gout is an independent risk factor for the occurrence of acute MI – particularly nonfatal acute MI – among young, low-risk patients suggests the need for "vigilant cardiovascular monitoring" of these patients, he stressed.
Dr. Kuo reported having no conflicts of interest to disclose.
LONDON – Gout is an independent risk factor for acute myocardial infarction, even among younger patients and those without cardiovascular risk factors, according to Dr. Chang-Fu Kuo, who presented a late-breaking report at the Annual European Congress of Rheumatology.
The risk for acute MI was 23% higher among gout patients than the general population, judging from an analysis of a large Taiwanese database. Among individuals aged 20-44 years old and those without additional cardiovascular risk factors, the risk of acute MI was increased by 59% and 76%, respectively, reported Dr. Kuo of Chang Gung Memorial Hospital, Taipei, Taiwan.
To investigate the risk of acute MI associated with gout, Dr. Kuo and colleagues analyzed the 2000 Taiwan National Health Insurance database, which is a representative sampling cohort of the general population. Specifically, the investigators compared rates of first hospital admission for acute MI among gout and nongout patients aged 20 years or older. Of the 704,503 individuals included in the cohort (mean age, 42.73 years), 26,566 were diagnosed and treated for gout in 1996-1999, Dr. Kuo said. Compared with the nongout patients, "the gout patients were significantly older, with a mean age of 55.4 years, and they were significantly more likely to have diabetes and hypertension," he said.
The investigators followed the cohort from January 2000 through December 2008, for a total of 5.6 million patient-years of follow-up. During this period, 3,718 patients were hospitalized for acute MI, including 463 patients with gout. Of these events, 299 were fatal, including 35 in gout patients, Dr. Kuo said. "The incidence of acute [MI] in gout patients was 2.20 per 1,000 patient years and was significantly higher than in nongout patients, which was 0.60," he said.
In the multivariate model adjusted for age, sex, diabetes, hypertension, coronary heart disease, stroke, and end-stage renal disease, the respective hazard ratios for all acute MI and nonfatal acute MI in gout patients were 1.23 and 1.26, Dr. Kuo reported. "In patients without cardiovascular risk factors, the hazard ratio for all acute [MI] was 1.84, and for nonfatal acute [MI] was 1.80," he said, and when assessed by age, the respective hazard ratios for gout patients aged 20-44 years, 45-59 years, and 60 years or older were 1.59, 1.24, and 1.11.
The multivariate model was not adjusted for hyperlipidemia, which has been associated with gout, Dr. Kuo said, acknowledging that elevated lipid levels could play an important role in the increased cardiovascular risks observed in the gout patients.
Although the increased risk of acute MI associated with gout has been previously reported, "the risk in younger patients and those with low risk profiles hasn’t previously been established," Dr. Kuo explained. The finding that gout is an independent risk factor for the occurrence of acute MI – particularly nonfatal acute MI – among young, low-risk patients suggests the need for "vigilant cardiovascular monitoring" of these patients, he stressed.
Dr. Kuo reported having no conflicts of interest to disclose.
FROM THE ANNUAL EUROPEAN CONGRESS OF RHEUMATOLOGY
Major Finding: The incidence of acute MI was increased by 76% in people aged 20-44 years who had no other cardiac risk factors except gout, compared with the general population.
Data Source: A representative sampling cohort representing 1 million randomly selected subjects from the general population of Taiwan.
Disclosures: Dr. Kuo reported having no conflicts to disclose.
HPV Vaccine Does Not Induce Lupus Flares : Vaccination did not change patients' anti-dsDNA titers, C3 or C4 levels, or SLEDAI or PGA scores.
Major Finding: The HPV vaccine does not exacerbate disease activity in women with SLE. The baseline, 3-month, and 6-month measures of disease activity were: C3: 0.79, 0.80, and 0.81 g/dL; C4: 0.15, 0.15, and 0.15 g/dL; anti-dsDNA: 131, 130, and 139 IU/mL; SLEDAI: 3.4, 3.4, and 3.0; and PGA: 0.26, 0.28, and 0.22.
Data Source: A prospective study of 50 female SLE patients and an unvaccinated cohort of SLE patients who were observed over a 5-year period at the same institution.
Disclosures: Dr. Mok disclosed having no financial conflicts of interest.
LONDON – The quadrivalent human papillomavirus vaccine is safe for patients with systemic lupus erythematosus and should be considered for women with inactive disease who receive stable doses of standard immunomodulatory therapy, according to Dr. Chi Chiu Mok.
Multiple studies have demonstrated higher rates of persistent HPV infections and precancerous lesions in women with SLE, compared with women in the general population, said Dr. Mok.
It has been hypothesized that immune dysfunction related to SLE or to treatment-induced immune suppression may prevent patients with the condition from being able to produce an effective immune response to the vaccine, and could possibly lead to disease flares or the production of new autoantibodies, Dr. Mo explained.
The recombinant quadrivalent HPV vaccine (Gardisil) provides protection against infection of the HPV serotypes 6, 11, 16, and 18, and it has been demonstrated to be safe and efficacious in female patients in the general population aged 9-26 years, according to Dr. Mok. Along with colleagues at Tuen Mun Hospital in Hong Kong, Dr. Mok evaluated the vaccine's safety and immunogen-icity in a cohort of SLE patients.
Toward this end, the investigators recruited 50 female patients aged 18–35 years who fulfilled at least four American College of Rheumatology criteria for SLE, and who had received a stable dose of prednisolone or other immunosuppressive agent within the previous 3 months, to participate in the prospective investigation. The mean age of the study participants was 25.8 years, and their mean disease duration was 6.6 years, he reported.
All of the study subjects received intramuscular injections of the vaccine and were evaluated at baseline and at 2 and 6 months post vaccination via the SLEDAI (SLE Disease Activity Index), PGA (Physicians' Global Assessment), and the SELENA (Safety of Estrogens in Lupus Erythematosus – National Assessment) disease flare index. Additionally, complement levels (C3 and C4) and anti-dsDNA (anti–double-stranded DNA) titers were assessed and patient-reported adverse events were recorded at the same time points, said Dr. Mok. With respect to baseline disease characteristics, the median SLEDAI score was 4; the mean anti-dsDNA titers, C3 levels, and C4 levels were 139 IU/mL, 0.81 g/dL, and 0.15 g/dL, respectively; and none of the patients had SELENA flares at baseline compared to preceding status, he said.
There were no significant changes in anti-dsDNA titers, C3 or C4 levels, or SLEDAI and PGA scores at any of the time points, Dr. Mok reported. Specifically, the baseline, 3-month, and 6-month measures of disease activity were: C3: 0.79, 0.80, and 0.81 g/dL; C4: 0.15, 0.15, and 0.15 g/dL; anti-dsDNA: 131, 130, and 139 IU/mL; SLEDAI: 3.4, 3.4, and 3.0; and PGA: 0.26, 0.28, and 0.22. “There were three mild to moderate mucocutaneous flares during the study period (one at month 2 and two at month 6), all of which were controlled with usual treatment,” he said.
“It's unclear whether a causal relationship exists between the vaccination and the three lupus flares, but the rate of flares [0.08 per patient per year] was lower than the rate observed in our lupus cohort during the previous 5 years [0.10 per patient per year], and no other adverse events associated with the vaccination were reported.”
The study findings indicate that the vaccine is safe in SLE patients, and the lack of significant alterations in the various SLE antibody measures suggests it does not induce an increased incidence of lupus flares, Dr. Mok stated.
Major Finding: The HPV vaccine does not exacerbate disease activity in women with SLE. The baseline, 3-month, and 6-month measures of disease activity were: C3: 0.79, 0.80, and 0.81 g/dL; C4: 0.15, 0.15, and 0.15 g/dL; anti-dsDNA: 131, 130, and 139 IU/mL; SLEDAI: 3.4, 3.4, and 3.0; and PGA: 0.26, 0.28, and 0.22.
Data Source: A prospective study of 50 female SLE patients and an unvaccinated cohort of SLE patients who were observed over a 5-year period at the same institution.
Disclosures: Dr. Mok disclosed having no financial conflicts of interest.
LONDON – The quadrivalent human papillomavirus vaccine is safe for patients with systemic lupus erythematosus and should be considered for women with inactive disease who receive stable doses of standard immunomodulatory therapy, according to Dr. Chi Chiu Mok.
Multiple studies have demonstrated higher rates of persistent HPV infections and precancerous lesions in women with SLE, compared with women in the general population, said Dr. Mok.
It has been hypothesized that immune dysfunction related to SLE or to treatment-induced immune suppression may prevent patients with the condition from being able to produce an effective immune response to the vaccine, and could possibly lead to disease flares or the production of new autoantibodies, Dr. Mo explained.
The recombinant quadrivalent HPV vaccine (Gardisil) provides protection against infection of the HPV serotypes 6, 11, 16, and 18, and it has been demonstrated to be safe and efficacious in female patients in the general population aged 9-26 years, according to Dr. Mok. Along with colleagues at Tuen Mun Hospital in Hong Kong, Dr. Mok evaluated the vaccine's safety and immunogen-icity in a cohort of SLE patients.
Toward this end, the investigators recruited 50 female patients aged 18–35 years who fulfilled at least four American College of Rheumatology criteria for SLE, and who had received a stable dose of prednisolone or other immunosuppressive agent within the previous 3 months, to participate in the prospective investigation. The mean age of the study participants was 25.8 years, and their mean disease duration was 6.6 years, he reported.
All of the study subjects received intramuscular injections of the vaccine and were evaluated at baseline and at 2 and 6 months post vaccination via the SLEDAI (SLE Disease Activity Index), PGA (Physicians' Global Assessment), and the SELENA (Safety of Estrogens in Lupus Erythematosus – National Assessment) disease flare index. Additionally, complement levels (C3 and C4) and anti-dsDNA (anti–double-stranded DNA) titers were assessed and patient-reported adverse events were recorded at the same time points, said Dr. Mok. With respect to baseline disease characteristics, the median SLEDAI score was 4; the mean anti-dsDNA titers, C3 levels, and C4 levels were 139 IU/mL, 0.81 g/dL, and 0.15 g/dL, respectively; and none of the patients had SELENA flares at baseline compared to preceding status, he said.
There were no significant changes in anti-dsDNA titers, C3 or C4 levels, or SLEDAI and PGA scores at any of the time points, Dr. Mok reported. Specifically, the baseline, 3-month, and 6-month measures of disease activity were: C3: 0.79, 0.80, and 0.81 g/dL; C4: 0.15, 0.15, and 0.15 g/dL; anti-dsDNA: 131, 130, and 139 IU/mL; SLEDAI: 3.4, 3.4, and 3.0; and PGA: 0.26, 0.28, and 0.22. “There were three mild to moderate mucocutaneous flares during the study period (one at month 2 and two at month 6), all of which were controlled with usual treatment,” he said.
“It's unclear whether a causal relationship exists between the vaccination and the three lupus flares, but the rate of flares [0.08 per patient per year] was lower than the rate observed in our lupus cohort during the previous 5 years [0.10 per patient per year], and no other adverse events associated with the vaccination were reported.”
The study findings indicate that the vaccine is safe in SLE patients, and the lack of significant alterations in the various SLE antibody measures suggests it does not induce an increased incidence of lupus flares, Dr. Mok stated.
Major Finding: The HPV vaccine does not exacerbate disease activity in women with SLE. The baseline, 3-month, and 6-month measures of disease activity were: C3: 0.79, 0.80, and 0.81 g/dL; C4: 0.15, 0.15, and 0.15 g/dL; anti-dsDNA: 131, 130, and 139 IU/mL; SLEDAI: 3.4, 3.4, and 3.0; and PGA: 0.26, 0.28, and 0.22.
Data Source: A prospective study of 50 female SLE patients and an unvaccinated cohort of SLE patients who were observed over a 5-year period at the same institution.
Disclosures: Dr. Mok disclosed having no financial conflicts of interest.
LONDON – The quadrivalent human papillomavirus vaccine is safe for patients with systemic lupus erythematosus and should be considered for women with inactive disease who receive stable doses of standard immunomodulatory therapy, according to Dr. Chi Chiu Mok.
Multiple studies have demonstrated higher rates of persistent HPV infections and precancerous lesions in women with SLE, compared with women in the general population, said Dr. Mok.
It has been hypothesized that immune dysfunction related to SLE or to treatment-induced immune suppression may prevent patients with the condition from being able to produce an effective immune response to the vaccine, and could possibly lead to disease flares or the production of new autoantibodies, Dr. Mo explained.
The recombinant quadrivalent HPV vaccine (Gardisil) provides protection against infection of the HPV serotypes 6, 11, 16, and 18, and it has been demonstrated to be safe and efficacious in female patients in the general population aged 9-26 years, according to Dr. Mok. Along with colleagues at Tuen Mun Hospital in Hong Kong, Dr. Mok evaluated the vaccine's safety and immunogen-icity in a cohort of SLE patients.
Toward this end, the investigators recruited 50 female patients aged 18–35 years who fulfilled at least four American College of Rheumatology criteria for SLE, and who had received a stable dose of prednisolone or other immunosuppressive agent within the previous 3 months, to participate in the prospective investigation. The mean age of the study participants was 25.8 years, and their mean disease duration was 6.6 years, he reported.
All of the study subjects received intramuscular injections of the vaccine and were evaluated at baseline and at 2 and 6 months post vaccination via the SLEDAI (SLE Disease Activity Index), PGA (Physicians' Global Assessment), and the SELENA (Safety of Estrogens in Lupus Erythematosus – National Assessment) disease flare index. Additionally, complement levels (C3 and C4) and anti-dsDNA (anti–double-stranded DNA) titers were assessed and patient-reported adverse events were recorded at the same time points, said Dr. Mok. With respect to baseline disease characteristics, the median SLEDAI score was 4; the mean anti-dsDNA titers, C3 levels, and C4 levels were 139 IU/mL, 0.81 g/dL, and 0.15 g/dL, respectively; and none of the patients had SELENA flares at baseline compared to preceding status, he said.
There were no significant changes in anti-dsDNA titers, C3 or C4 levels, or SLEDAI and PGA scores at any of the time points, Dr. Mok reported. Specifically, the baseline, 3-month, and 6-month measures of disease activity were: C3: 0.79, 0.80, and 0.81 g/dL; C4: 0.15, 0.15, and 0.15 g/dL; anti-dsDNA: 131, 130, and 139 IU/mL; SLEDAI: 3.4, 3.4, and 3.0; and PGA: 0.26, 0.28, and 0.22. “There were three mild to moderate mucocutaneous flares during the study period (one at month 2 and two at month 6), all of which were controlled with usual treatment,” he said.
“It's unclear whether a causal relationship exists between the vaccination and the three lupus flares, but the rate of flares [0.08 per patient per year] was lower than the rate observed in our lupus cohort during the previous 5 years [0.10 per patient per year], and no other adverse events associated with the vaccination were reported.”
The study findings indicate that the vaccine is safe in SLE patients, and the lack of significant alterations in the various SLE antibody measures suggests it does not induce an increased incidence of lupus flares, Dr. Mok stated.
RA, Diabetes Confer Same Cardiovascular Risk
Major Finding: The RA and diabetes cohorts both had a 1.7 increased incidence rate ratio (IRR) of MI, compared with the general population.
Data Source: A large, population-based study of the incidence of new-onset rheumatoid arthritis, diabetes, and myocardial infarction using Danish patient registry information covering a 10-year period.
Disclosures: The study was supported by an unrestricted grant from the Danish Rheumatism Association. The authors disclosed having no conflicts of interest.
The cardiovascular risk in rheumatoid arthritis is comparable to that of diabetes, a large Danish study has shown.
Further, the risk of myocardial infarction (MI) in rheumatoid arthritis patients corresponds to that observed in the general population of individuals without the musculoskeletal condition who are, on average, 10 years older and does not appear to be affected by the duration of drug treatment for the disease, Dr. Jesper Lindhardsen of Gentofte University Hospital in Copenhagen, and colleagues reported.
Using nationwide registers encompassing the entire Danish population older than 16 years, the investigators identified individuals with new-onset rheumatoid arthritis (RA), new-onset diabetes, and new MI during a 10-year period, excluding individuals with prior disease and incomplete data entries from the full cohort of 4,311,022 subjects, they wrote.
During the 10-year study period, 9,921 individuals developed RA and 129,659 developed diabetes. Compared with the diabetes patients, “RA patients were more often women, used less cardioprotective medications, and had less comorbidity, whereas age was similar in the two groups,” they reported.
Regarding cardiovascular outcomes, 265 of the RA patients and 3,948 of the diabetes patients had new MI, representing in both cohorts a 1.7 increased incidence rate ratio (IRR) of MI in a fully adjusted model compared with the general population in which 75,870 individuals had new myocardial infarctions. The IRR among patients with both RA and diabetes was 2.6, “which roughly equaled the predicted additive risk for the two separate diseases, they wrote (Ann. Rheum. Dis. 2011;70:929–34).
The investigators conducted a nested case-control study that corroborated the comparable risk of MI in the RA and diabetes patients. The findings demonstrated that the increased risk in these groups was independent of treatment duration within the time frame of the current study, they wrote.
Stratified by gender, the MI risk estimates did not differ between women and men in the RA group. In the diabetes patients, however, women were at significantly higher risk than men for the adverse cardiovascular outcome, the authors wrote. An age-dependent pattern of MI risk was also observed. Specifically, among women with RA and diabetes, respectively, the risk of MI in those younger than 50 years old was 5.5 and 5.9 times that observed in the age-matched reference group, they reported. Additionally, for women between 50 and 65 years of age, the IRRs were 1.7 and 2.6 for RA and diabetes patients, respectively.
The age-stratified patterns observed in men were different, the authors stated, noting that “the IRRs in the two oldest age groups were comparable, and even tended to be slightly higher in the 50-65 years age group of RA patients compared to the same-aged [diabetes] patients.” And while the youngest men with RA had a markedly raised IRR, diabetes patients in the same age stratum had a significantly higher risk, with an IRR of 4.9 compared with 2.1, they said.
In a fully adjusted regression model in which the IRRs for MI in RA patients were calculated according to 10-year subject age intervals, “RA patients had the same, or higher, risk of MI as control subjects who were, on average, 10 years older,” the authors reported.
Although the study has several limitations, including the identification of RA patients based on dispensed prescriptions and diagnosis versus the 1987 American College of Rheumatology criteria, the reliance on the use of glucose-lowering drugs as a proxy for diabetes, and the lack of information about classic cardiovascular risk factors, “the results corroborate and expand previous findings in this area of research and indicate that patients with RA should be considered for more aggressive primary [cardiovascular disease] prevention,” the authors stressed.
In an accompanying editorial, Dr. Michael T. Nurmohamed and Dr. George Kitas of VU University Medical Centre in Amsterdam wrote that the findings of the current study should put to bed any doubt or debate about an enhanced cardiovascular risk in RA. “Importantly, they also provide further evidence that the cardiovascular risk in RA is broadly similar to that of contemporarily managed diabetes,” they stated. The results of the study, as well as the success of cardiovascular risk management in diabetes provides a clear incentive to identify and actively manage, if necessary, cardiovascular risk in all RA patients as part of quality routine rheumatological practice” (Ann. Rheum. Dis. 2011;70:881–3).
The study was sponsored by an unrestricted grant from the Danish Rheumatism Association. The authors of the study and the accompanying editorial reported having no conflicts of interest.
'RA patients had the same, or higher, risk of MI as control subjects who were, on average, 10 years older.'
Source DR. LINDHARDSEN
Major Finding: The RA and diabetes cohorts both had a 1.7 increased incidence rate ratio (IRR) of MI, compared with the general population.
Data Source: A large, population-based study of the incidence of new-onset rheumatoid arthritis, diabetes, and myocardial infarction using Danish patient registry information covering a 10-year period.
Disclosures: The study was supported by an unrestricted grant from the Danish Rheumatism Association. The authors disclosed having no conflicts of interest.
The cardiovascular risk in rheumatoid arthritis is comparable to that of diabetes, a large Danish study has shown.
Further, the risk of myocardial infarction (MI) in rheumatoid arthritis patients corresponds to that observed in the general population of individuals without the musculoskeletal condition who are, on average, 10 years older and does not appear to be affected by the duration of drug treatment for the disease, Dr. Jesper Lindhardsen of Gentofte University Hospital in Copenhagen, and colleagues reported.
Using nationwide registers encompassing the entire Danish population older than 16 years, the investigators identified individuals with new-onset rheumatoid arthritis (RA), new-onset diabetes, and new MI during a 10-year period, excluding individuals with prior disease and incomplete data entries from the full cohort of 4,311,022 subjects, they wrote.
During the 10-year study period, 9,921 individuals developed RA and 129,659 developed diabetes. Compared with the diabetes patients, “RA patients were more often women, used less cardioprotective medications, and had less comorbidity, whereas age was similar in the two groups,” they reported.
Regarding cardiovascular outcomes, 265 of the RA patients and 3,948 of the diabetes patients had new MI, representing in both cohorts a 1.7 increased incidence rate ratio (IRR) of MI in a fully adjusted model compared with the general population in which 75,870 individuals had new myocardial infarctions. The IRR among patients with both RA and diabetes was 2.6, “which roughly equaled the predicted additive risk for the two separate diseases, they wrote (Ann. Rheum. Dis. 2011;70:929–34).
The investigators conducted a nested case-control study that corroborated the comparable risk of MI in the RA and diabetes patients. The findings demonstrated that the increased risk in these groups was independent of treatment duration within the time frame of the current study, they wrote.
Stratified by gender, the MI risk estimates did not differ between women and men in the RA group. In the diabetes patients, however, women were at significantly higher risk than men for the adverse cardiovascular outcome, the authors wrote. An age-dependent pattern of MI risk was also observed. Specifically, among women with RA and diabetes, respectively, the risk of MI in those younger than 50 years old was 5.5 and 5.9 times that observed in the age-matched reference group, they reported. Additionally, for women between 50 and 65 years of age, the IRRs were 1.7 and 2.6 for RA and diabetes patients, respectively.
The age-stratified patterns observed in men were different, the authors stated, noting that “the IRRs in the two oldest age groups were comparable, and even tended to be slightly higher in the 50-65 years age group of RA patients compared to the same-aged [diabetes] patients.” And while the youngest men with RA had a markedly raised IRR, diabetes patients in the same age stratum had a significantly higher risk, with an IRR of 4.9 compared with 2.1, they said.
In a fully adjusted regression model in which the IRRs for MI in RA patients were calculated according to 10-year subject age intervals, “RA patients had the same, or higher, risk of MI as control subjects who were, on average, 10 years older,” the authors reported.
Although the study has several limitations, including the identification of RA patients based on dispensed prescriptions and diagnosis versus the 1987 American College of Rheumatology criteria, the reliance on the use of glucose-lowering drugs as a proxy for diabetes, and the lack of information about classic cardiovascular risk factors, “the results corroborate and expand previous findings in this area of research and indicate that patients with RA should be considered for more aggressive primary [cardiovascular disease] prevention,” the authors stressed.
In an accompanying editorial, Dr. Michael T. Nurmohamed and Dr. George Kitas of VU University Medical Centre in Amsterdam wrote that the findings of the current study should put to bed any doubt or debate about an enhanced cardiovascular risk in RA. “Importantly, they also provide further evidence that the cardiovascular risk in RA is broadly similar to that of contemporarily managed diabetes,” they stated. The results of the study, as well as the success of cardiovascular risk management in diabetes provides a clear incentive to identify and actively manage, if necessary, cardiovascular risk in all RA patients as part of quality routine rheumatological practice” (Ann. Rheum. Dis. 2011;70:881–3).
The study was sponsored by an unrestricted grant from the Danish Rheumatism Association. The authors of the study and the accompanying editorial reported having no conflicts of interest.
'RA patients had the same, or higher, risk of MI as control subjects who were, on average, 10 years older.'
Source DR. LINDHARDSEN
Major Finding: The RA and diabetes cohorts both had a 1.7 increased incidence rate ratio (IRR) of MI, compared with the general population.
Data Source: A large, population-based study of the incidence of new-onset rheumatoid arthritis, diabetes, and myocardial infarction using Danish patient registry information covering a 10-year period.
Disclosures: The study was supported by an unrestricted grant from the Danish Rheumatism Association. The authors disclosed having no conflicts of interest.
The cardiovascular risk in rheumatoid arthritis is comparable to that of diabetes, a large Danish study has shown.
Further, the risk of myocardial infarction (MI) in rheumatoid arthritis patients corresponds to that observed in the general population of individuals without the musculoskeletal condition who are, on average, 10 years older and does not appear to be affected by the duration of drug treatment for the disease, Dr. Jesper Lindhardsen of Gentofte University Hospital in Copenhagen, and colleagues reported.
Using nationwide registers encompassing the entire Danish population older than 16 years, the investigators identified individuals with new-onset rheumatoid arthritis (RA), new-onset diabetes, and new MI during a 10-year period, excluding individuals with prior disease and incomplete data entries from the full cohort of 4,311,022 subjects, they wrote.
During the 10-year study period, 9,921 individuals developed RA and 129,659 developed diabetes. Compared with the diabetes patients, “RA patients were more often women, used less cardioprotective medications, and had less comorbidity, whereas age was similar in the two groups,” they reported.
Regarding cardiovascular outcomes, 265 of the RA patients and 3,948 of the diabetes patients had new MI, representing in both cohorts a 1.7 increased incidence rate ratio (IRR) of MI in a fully adjusted model compared with the general population in which 75,870 individuals had new myocardial infarctions. The IRR among patients with both RA and diabetes was 2.6, “which roughly equaled the predicted additive risk for the two separate diseases, they wrote (Ann. Rheum. Dis. 2011;70:929–34).
The investigators conducted a nested case-control study that corroborated the comparable risk of MI in the RA and diabetes patients. The findings demonstrated that the increased risk in these groups was independent of treatment duration within the time frame of the current study, they wrote.
Stratified by gender, the MI risk estimates did not differ between women and men in the RA group. In the diabetes patients, however, women were at significantly higher risk than men for the adverse cardiovascular outcome, the authors wrote. An age-dependent pattern of MI risk was also observed. Specifically, among women with RA and diabetes, respectively, the risk of MI in those younger than 50 years old was 5.5 and 5.9 times that observed in the age-matched reference group, they reported. Additionally, for women between 50 and 65 years of age, the IRRs were 1.7 and 2.6 for RA and diabetes patients, respectively.
The age-stratified patterns observed in men were different, the authors stated, noting that “the IRRs in the two oldest age groups were comparable, and even tended to be slightly higher in the 50-65 years age group of RA patients compared to the same-aged [diabetes] patients.” And while the youngest men with RA had a markedly raised IRR, diabetes patients in the same age stratum had a significantly higher risk, with an IRR of 4.9 compared with 2.1, they said.
In a fully adjusted regression model in which the IRRs for MI in RA patients were calculated according to 10-year subject age intervals, “RA patients had the same, or higher, risk of MI as control subjects who were, on average, 10 years older,” the authors reported.
Although the study has several limitations, including the identification of RA patients based on dispensed prescriptions and diagnosis versus the 1987 American College of Rheumatology criteria, the reliance on the use of glucose-lowering drugs as a proxy for diabetes, and the lack of information about classic cardiovascular risk factors, “the results corroborate and expand previous findings in this area of research and indicate that patients with RA should be considered for more aggressive primary [cardiovascular disease] prevention,” the authors stressed.
In an accompanying editorial, Dr. Michael T. Nurmohamed and Dr. George Kitas of VU University Medical Centre in Amsterdam wrote that the findings of the current study should put to bed any doubt or debate about an enhanced cardiovascular risk in RA. “Importantly, they also provide further evidence that the cardiovascular risk in RA is broadly similar to that of contemporarily managed diabetes,” they stated. The results of the study, as well as the success of cardiovascular risk management in diabetes provides a clear incentive to identify and actively manage, if necessary, cardiovascular risk in all RA patients as part of quality routine rheumatological practice” (Ann. Rheum. Dis. 2011;70:881–3).
The study was sponsored by an unrestricted grant from the Danish Rheumatism Association. The authors of the study and the accompanying editorial reported having no conflicts of interest.
'RA patients had the same, or higher, risk of MI as control subjects who were, on average, 10 years older.'
Source DR. LINDHARDSEN
CCSVI Controversy: A Call for New Research
Multiple sclerosis patients and endovascular interventionalists were elated when Italian researchers reported in 2009 that they had found evidence of chronic cerebrospinal venous insufficiency in nearly every MS patient they had studied and that in many cases, balloon angioplasty and sometimes stent placement of central thoracic veins reduced or eliminated signs of the disease. Neurologists, on the other hand, suggested that hope might be eclipsing reason in the rush to advocate the vascular procedure, given the single-center study's small sample size and nonrandomized, uncontrolled design.
The opposing perspectives incited an apparent turf war within the MS community fueled by accusations on both sides, according to Dr. Jack Burks, chief medical officer of the Multiple Sclerosis Association of America. At issue, he said, is the validity not only of the study results but also of the underlying hypothesis that toxic iron overload in the brain due to chronic cerebrospinal venous insufficiency (CCSVI) might have a primary role in the pathogenesis of MS - a hypothesis that contradicts the compelling body of evidence suggesting that MS is primarily an autoimmune condition.
On one side of the debate are the MS patients and endovascular interventionalists, dubbed the "liberators" by Dr. Burks because of their unflappable advocacy for what has become known as the liberation procedure - the endovascular surgery designed to open the lesions causing the venous insufficiency, he said.
"Neurologists believe the interventionalists are overstating the possible value of CCSVI and that commercial interests are overriding scientific inquiry," according to Dr. Burks, a neurologist and clinical professor of medicine at the University of Nevada, Reno. Patients, armed with anecdotal evidence downloaded from the Internet, are certain that CCSVI surgery is the miracle they've been waiting for and perceive the hesitancy of U.S. and Canadian neurologists to embrace the treatment as evidence of a possible conspiracy with pharmaceutical companies who stand to lose billions of dollars if the surgery becomes a first-line treatment, he said. Further, he noted, advocates of CCSVI claim that neurologists who refuse patients' demands for diagnostic testing and surgical referral for CCSVI are jeopardizing the safety of those patients, who are traveling to foreign countries to get the care that they cannot receive in North America.
To date, the majority of the evidence regarding CCSVI diagnosis and treatment in MS is inconsistent, and can be confusing, Dr. Burks noted. In the initial study, Dr. Paolo Zamboni of the University of Ferrara in Italy, and colleagues, used Doppler ultrasound to examine venous drainage of the brain and spinal cord in 65 patients with different types of MS and 235 controls without MS and observed abnormal venous flow in all of the MS patients and none of the controls. The patterns of venous obstruction differed depending on MS stage and course, although there was no apparent relationship between disease severity and extent of venous obstruction, and MS treatment status did not influence the signs of CCSVI in any of the patients, the authors wrote (J. Neurol. Neurosurg. Psychiatry 2009;80:392-9).
The researchers went on to conduct an open pilot study to determine whether percutaneous transluminal angioplasty could safely and effectively treat the narrowing of the extracranial cerebrospinal veins in the 65 MS patients in which the condition was observed - 35 with relapsing-remitting MS, 20 with secondary progressive MS, and 10 with primary progressive MS. They reported significant improvements in MS clinical outcome measures, significant reductions in new brain lesions on MRI, and significant reductions in the number of relapses experienced by some of the patients.
The findings were limited, however, not only by the study design, but also by the fact that patients remained on their disease-modifying antirheumatic drug therapy during the study period and the timing and type of MRI scans varied among the patients, according to the authors. They also noted that restenosis of the internal jugular veins occurred in nearly half of the patients (J. Vasc. Surg. 2009;50:1348-58).
Since the initial paper, a number of CCSVI studies of various designs have been undertaken, with contradictory results. Following are some of the investigations reported within the past year:
P Researchers at the University of Buffalo found that up to 62% of the 280 patients with MS enrolled in the Combined Transcranial and Extracranial Venous Doppler Evaluation study - the first randomized clinical trial to evaluate MS patients for CCSVI - had the characteristic narrowing of the extracranial veins compared with approximately 22% of 220 healthy controls. While the results, which were reported at the annual meeting of the American Academy of Neurology, did not establish causation, they showed "that narrowing of the extracranial veins, at the very least, is an important association in multiple sclerosis," principal investigator Dr. Robert Zivadinov said in a statement. He acknowledged that the finding of vascular narrowing in nearly a quarter of the healthy controls warranted additional investigation (www.buffalo.edu/news/fast-execute.cgi/article-page.html?article=109370009).
P In an open-label study of extracranial Doppler criteria of CCSVI in 70 MS patients in Poland - 49 with relapsing-remitting MS, 5 with primary progressive MS, and 16 with secondary progressive MS - investigators detected at least two of four extracranial criteria in 90% of the patients. They concluded that, while the extracranial abnormalities could exist in various combinations, "the most common pathology in our patients was the presence of an inverted valve or another pathologic structure [like membranaceous or netlike septum] in the area of junction of the [internal jugular vein] with the brachiocephalic vein (Int. Angiol. 2010;29:109-14).
P A comparison of the internal jugular vein hemodynamics and morphology in 25 patients with MS and 25 controls identified abnormal findings in 92% of the MS patients and 24% of the controls, and evidence of CCSVI in 84% of the MS patients and none of the controls, leading the investigators to conclude that both hemodynamic abnormalities and morphologic changes in the internal jugular vein "are strongly associated with MS" (Int. Angiol. 2010;29:115-20).
P An extended extra- and transcranial color-coded sonography study in 56 MS patients and 20 controls detected no internal jugular vein stenosis and normal blood flow direction in all but 1 patient. There were no between-group differences in intracranial veins and during Valsalva maneuver, and none of the patients fulfilled more than one CCSVI criterion, according to the authors. They concluded that their findings "challenge the hypothesis that cerebral venous congestion plays a significant role in the pathogenesis of MS" (Ann. Neurol. 2010;68:173-83).
P Swedish investigators used phase-contrast MRI to study 21 relapsing-remitting MS patients and 20 healthy controls and found no differences in internal jugular venous outflow, aqueductal cerebrospinal fluid flow, or the presence of internal jugular blood reflux between the two groups. Although contrast-enhanced MR angiography showed internal jugular vein stenosis in 3 of the 21 MS patients, the authors stated they found no evidence "confirming the suggested vascular multiple sclerosis hypothesis" (Ann. Neurol. 2010;68:255-9).
P The authors of an MR venography and flow quantification study in The Netherlands compared the intracranial and extracranial venous anatomy and the intracerebral venous flow profiles of 20 MS patients and 20 age- and gender-matched controls, with image analysis performed by blinded interventional neuroradiologists. They identified venous system anomalies in 50% of the MS patients and 40% of the healthy controls and no venous backflow in either group. "Given the normal intracranial venous flow quantification results, it is likely that these findings reflect anatomical variants of venous drainage rather than clinically relevant venous outflow obstructions," the authors wrote (J. Neurol. Neurosurg. Psychiatry 2010 Oct. 27 [doi: 10.1136/jnnp.2010.223479]).
P Italian researchers investigating the occurrence of CCSVI in 50 consecutive patients with clinically isolated syndromes suggestive of MS reviewed the patients' extracranial and transcranial venous echo-color Doppler sonographs and compared the findings to those of 50 age- and gender-matched healthy controls as well as those of 60 patients with transient global amnesia (TGA) and 60 healthy controls matched to the TGA patients. They found extracranial Doppler sonographic abnormalities in 52% of patients with possible MS, 68.3% of patients with TGA, and 31.8% of the healthy controls. While eight of the patients with possible MS fulfilled the CCSVI criteria, selective phlebography showed no venous anomalies in seven of them. The authors concluded that there was no evidence of CCSVI at MS onset but recommended further studies to "clarify whether CCSVI is associated with later disease stages and characterizes the progressive forms of MS" (Ann. Neurol. 2011;69:90-9).
In a position statement, the Society of Interventional Radiology stated that at present, the published literature is "inconclusive on whether CCSVI is a clinically important factor and on whether balloon angioplasty and/or stent placement are effective in patients with MS" (J. Vasc. Interv. Radiol. 2010;21:1335-7).
Additionally, in a commentary on the treatment of CCSVI, representatives of the Cardiovascular and Interventional Radiological Society of Europe acknowledged that although several centers worldwide are promoting and performing balloon dilatation, with or without stenting for CCSVI, "We believe that until real scientific data are available for CCSVI and balloon dilatation, this treatment should not be offered to MS patients outside of a well designed clinical trial" (Cardiovasc. Intervent. Radiol. 2011;34:1-2).
Toward that end, the National Multiple Sclerosis Society of the United States and the MS Society of Canada have pledged $2.4 million in support of seven CCSVI research studies, including projects designed to evaluate venous abnormalities in children and teens with MS, patients with early and late stage MS, and those at risk for MS.
An international review panel comprising radiologists, vascular surgeons, and neurologists evaluated research applications via an expedited review process, according to the societies.
Dr. Burks disclosed relationships with various pharmaceutical companies. Dr. Baracchini had no relevant conflicts.
To say that the relationship between CCSVI and multiple sclerosis is controversial is an understatement. This article introduces both sides of the story and summarizes the current evidence. While many physicians remain understandably skeptical, it is worth remembering that "conventional wisdom" on the pathophysiology of some diseases has turned out to be way off the mark - consider peptic ulcers. Clearly, more objective data is needed before routine interventions for CCSVI can be recommended, and hopefully, ongoing registries and trials will provide that data. In the meantime, those of us involved with the vascular laboratory should be prepared to evaluate patients for the abnormalities described in CCSVI. Detection of reflux and obstruction in the internal jugular and vertebral veins by duplex ultrasound (in both supine and seated positions) is based on the same general principles as the more familiar upper extremity venous and carotid duplex examinations. Ideally, patients should be screened and entered into a clinical study to establish an evidence base for future decision-making. Until then, we will be stuck between the "liberators" and the "nihilists", and our patients will be caught in the middle.
Robert Eugene Zierler, M.D., is professor of surgery, division of vascular surgery, department of surgery, and medical director, Vascular Diagnostic Service, University of Washington School of Medicine, Seattle, Wash. He is also an associate medical editor for Vascular Specialist.
To say that the relationship between CCSVI and multiple sclerosis is controversial is an understatement. This article introduces both sides of the story and summarizes the current evidence. While many physicians remain understandably skeptical, it is worth remembering that "conventional wisdom" on the pathophysiology of some diseases has turned out to be way off the mark - consider peptic ulcers. Clearly, more objective data is needed before routine interventions for CCSVI can be recommended, and hopefully, ongoing registries and trials will provide that data. In the meantime, those of us involved with the vascular laboratory should be prepared to evaluate patients for the abnormalities described in CCSVI. Detection of reflux and obstruction in the internal jugular and vertebral veins by duplex ultrasound (in both supine and seated positions) is based on the same general principles as the more familiar upper extremity venous and carotid duplex examinations. Ideally, patients should be screened and entered into a clinical study to establish an evidence base for future decision-making. Until then, we will be stuck between the "liberators" and the "nihilists", and our patients will be caught in the middle.
Robert Eugene Zierler, M.D., is professor of surgery, division of vascular surgery, department of surgery, and medical director, Vascular Diagnostic Service, University of Washington School of Medicine, Seattle, Wash. He is also an associate medical editor for Vascular Specialist.
To say that the relationship between CCSVI and multiple sclerosis is controversial is an understatement. This article introduces both sides of the story and summarizes the current evidence. While many physicians remain understandably skeptical, it is worth remembering that "conventional wisdom" on the pathophysiology of some diseases has turned out to be way off the mark - consider peptic ulcers. Clearly, more objective data is needed before routine interventions for CCSVI can be recommended, and hopefully, ongoing registries and trials will provide that data. In the meantime, those of us involved with the vascular laboratory should be prepared to evaluate patients for the abnormalities described in CCSVI. Detection of reflux and obstruction in the internal jugular and vertebral veins by duplex ultrasound (in both supine and seated positions) is based on the same general principles as the more familiar upper extremity venous and carotid duplex examinations. Ideally, patients should be screened and entered into a clinical study to establish an evidence base for future decision-making. Until then, we will be stuck between the "liberators" and the "nihilists", and our patients will be caught in the middle.
Robert Eugene Zierler, M.D., is professor of surgery, division of vascular surgery, department of surgery, and medical director, Vascular Diagnostic Service, University of Washington School of Medicine, Seattle, Wash. He is also an associate medical editor for Vascular Specialist.
Multiple sclerosis patients and endovascular interventionalists were elated when Italian researchers reported in 2009 that they had found evidence of chronic cerebrospinal venous insufficiency in nearly every MS patient they had studied and that in many cases, balloon angioplasty and sometimes stent placement of central thoracic veins reduced or eliminated signs of the disease. Neurologists, on the other hand, suggested that hope might be eclipsing reason in the rush to advocate the vascular procedure, given the single-center study's small sample size and nonrandomized, uncontrolled design.
The opposing perspectives incited an apparent turf war within the MS community fueled by accusations on both sides, according to Dr. Jack Burks, chief medical officer of the Multiple Sclerosis Association of America. At issue, he said, is the validity not only of the study results but also of the underlying hypothesis that toxic iron overload in the brain due to chronic cerebrospinal venous insufficiency (CCSVI) might have a primary role in the pathogenesis of MS - a hypothesis that contradicts the compelling body of evidence suggesting that MS is primarily an autoimmune condition.
On one side of the debate are the MS patients and endovascular interventionalists, dubbed the "liberators" by Dr. Burks because of their unflappable advocacy for what has become known as the liberation procedure - the endovascular surgery designed to open the lesions causing the venous insufficiency, he said.
"Neurologists believe the interventionalists are overstating the possible value of CCSVI and that commercial interests are overriding scientific inquiry," according to Dr. Burks, a neurologist and clinical professor of medicine at the University of Nevada, Reno. Patients, armed with anecdotal evidence downloaded from the Internet, are certain that CCSVI surgery is the miracle they've been waiting for and perceive the hesitancy of U.S. and Canadian neurologists to embrace the treatment as evidence of a possible conspiracy with pharmaceutical companies who stand to lose billions of dollars if the surgery becomes a first-line treatment, he said. Further, he noted, advocates of CCSVI claim that neurologists who refuse patients' demands for diagnostic testing and surgical referral for CCSVI are jeopardizing the safety of those patients, who are traveling to foreign countries to get the care that they cannot receive in North America.
To date, the majority of the evidence regarding CCSVI diagnosis and treatment in MS is inconsistent, and can be confusing, Dr. Burks noted. In the initial study, Dr. Paolo Zamboni of the University of Ferrara in Italy, and colleagues, used Doppler ultrasound to examine venous drainage of the brain and spinal cord in 65 patients with different types of MS and 235 controls without MS and observed abnormal venous flow in all of the MS patients and none of the controls. The patterns of venous obstruction differed depending on MS stage and course, although there was no apparent relationship between disease severity and extent of venous obstruction, and MS treatment status did not influence the signs of CCSVI in any of the patients, the authors wrote (J. Neurol. Neurosurg. Psychiatry 2009;80:392-9).
The researchers went on to conduct an open pilot study to determine whether percutaneous transluminal angioplasty could safely and effectively treat the narrowing of the extracranial cerebrospinal veins in the 65 MS patients in which the condition was observed - 35 with relapsing-remitting MS, 20 with secondary progressive MS, and 10 with primary progressive MS. They reported significant improvements in MS clinical outcome measures, significant reductions in new brain lesions on MRI, and significant reductions in the number of relapses experienced by some of the patients.
The findings were limited, however, not only by the study design, but also by the fact that patients remained on their disease-modifying antirheumatic drug therapy during the study period and the timing and type of MRI scans varied among the patients, according to the authors. They also noted that restenosis of the internal jugular veins occurred in nearly half of the patients (J. Vasc. Surg. 2009;50:1348-58).
Since the initial paper, a number of CCSVI studies of various designs have been undertaken, with contradictory results. Following are some of the investigations reported within the past year:
P Researchers at the University of Buffalo found that up to 62% of the 280 patients with MS enrolled in the Combined Transcranial and Extracranial Venous Doppler Evaluation study - the first randomized clinical trial to evaluate MS patients for CCSVI - had the characteristic narrowing of the extracranial veins compared with approximately 22% of 220 healthy controls. While the results, which were reported at the annual meeting of the American Academy of Neurology, did not establish causation, they showed "that narrowing of the extracranial veins, at the very least, is an important association in multiple sclerosis," principal investigator Dr. Robert Zivadinov said in a statement. He acknowledged that the finding of vascular narrowing in nearly a quarter of the healthy controls warranted additional investigation (www.buffalo.edu/news/fast-execute.cgi/article-page.html?article=109370009).
P In an open-label study of extracranial Doppler criteria of CCSVI in 70 MS patients in Poland - 49 with relapsing-remitting MS, 5 with primary progressive MS, and 16 with secondary progressive MS - investigators detected at least two of four extracranial criteria in 90% of the patients. They concluded that, while the extracranial abnormalities could exist in various combinations, "the most common pathology in our patients was the presence of an inverted valve or another pathologic structure [like membranaceous or netlike septum] in the area of junction of the [internal jugular vein] with the brachiocephalic vein (Int. Angiol. 2010;29:109-14).
P A comparison of the internal jugular vein hemodynamics and morphology in 25 patients with MS and 25 controls identified abnormal findings in 92% of the MS patients and 24% of the controls, and evidence of CCSVI in 84% of the MS patients and none of the controls, leading the investigators to conclude that both hemodynamic abnormalities and morphologic changes in the internal jugular vein "are strongly associated with MS" (Int. Angiol. 2010;29:115-20).
P An extended extra- and transcranial color-coded sonography study in 56 MS patients and 20 controls detected no internal jugular vein stenosis and normal blood flow direction in all but 1 patient. There were no between-group differences in intracranial veins and during Valsalva maneuver, and none of the patients fulfilled more than one CCSVI criterion, according to the authors. They concluded that their findings "challenge the hypothesis that cerebral venous congestion plays a significant role in the pathogenesis of MS" (Ann. Neurol. 2010;68:173-83).
P Swedish investigators used phase-contrast MRI to study 21 relapsing-remitting MS patients and 20 healthy controls and found no differences in internal jugular venous outflow, aqueductal cerebrospinal fluid flow, or the presence of internal jugular blood reflux between the two groups. Although contrast-enhanced MR angiography showed internal jugular vein stenosis in 3 of the 21 MS patients, the authors stated they found no evidence "confirming the suggested vascular multiple sclerosis hypothesis" (Ann. Neurol. 2010;68:255-9).
P The authors of an MR venography and flow quantification study in The Netherlands compared the intracranial and extracranial venous anatomy and the intracerebral venous flow profiles of 20 MS patients and 20 age- and gender-matched controls, with image analysis performed by blinded interventional neuroradiologists. They identified venous system anomalies in 50% of the MS patients and 40% of the healthy controls and no venous backflow in either group. "Given the normal intracranial venous flow quantification results, it is likely that these findings reflect anatomical variants of venous drainage rather than clinically relevant venous outflow obstructions," the authors wrote (J. Neurol. Neurosurg. Psychiatry 2010 Oct. 27 [doi: 10.1136/jnnp.2010.223479]).
P Italian researchers investigating the occurrence of CCSVI in 50 consecutive patients with clinically isolated syndromes suggestive of MS reviewed the patients' extracranial and transcranial venous echo-color Doppler sonographs and compared the findings to those of 50 age- and gender-matched healthy controls as well as those of 60 patients with transient global amnesia (TGA) and 60 healthy controls matched to the TGA patients. They found extracranial Doppler sonographic abnormalities in 52% of patients with possible MS, 68.3% of patients with TGA, and 31.8% of the healthy controls. While eight of the patients with possible MS fulfilled the CCSVI criteria, selective phlebography showed no venous anomalies in seven of them. The authors concluded that there was no evidence of CCSVI at MS onset but recommended further studies to "clarify whether CCSVI is associated with later disease stages and characterizes the progressive forms of MS" (Ann. Neurol. 2011;69:90-9).
In a position statement, the Society of Interventional Radiology stated that at present, the published literature is "inconclusive on whether CCSVI is a clinically important factor and on whether balloon angioplasty and/or stent placement are effective in patients with MS" (J. Vasc. Interv. Radiol. 2010;21:1335-7).
Additionally, in a commentary on the treatment of CCSVI, representatives of the Cardiovascular and Interventional Radiological Society of Europe acknowledged that although several centers worldwide are promoting and performing balloon dilatation, with or without stenting for CCSVI, "We believe that until real scientific data are available for CCSVI and balloon dilatation, this treatment should not be offered to MS patients outside of a well designed clinical trial" (Cardiovasc. Intervent. Radiol. 2011;34:1-2).
Toward that end, the National Multiple Sclerosis Society of the United States and the MS Society of Canada have pledged $2.4 million in support of seven CCSVI research studies, including projects designed to evaluate venous abnormalities in children and teens with MS, patients with early and late stage MS, and those at risk for MS.
An international review panel comprising radiologists, vascular surgeons, and neurologists evaluated research applications via an expedited review process, according to the societies.
Dr. Burks disclosed relationships with various pharmaceutical companies. Dr. Baracchini had no relevant conflicts.
Multiple sclerosis patients and endovascular interventionalists were elated when Italian researchers reported in 2009 that they had found evidence of chronic cerebrospinal venous insufficiency in nearly every MS patient they had studied and that in many cases, balloon angioplasty and sometimes stent placement of central thoracic veins reduced or eliminated signs of the disease. Neurologists, on the other hand, suggested that hope might be eclipsing reason in the rush to advocate the vascular procedure, given the single-center study's small sample size and nonrandomized, uncontrolled design.
The opposing perspectives incited an apparent turf war within the MS community fueled by accusations on both sides, according to Dr. Jack Burks, chief medical officer of the Multiple Sclerosis Association of America. At issue, he said, is the validity not only of the study results but also of the underlying hypothesis that toxic iron overload in the brain due to chronic cerebrospinal venous insufficiency (CCSVI) might have a primary role in the pathogenesis of MS - a hypothesis that contradicts the compelling body of evidence suggesting that MS is primarily an autoimmune condition.
On one side of the debate are the MS patients and endovascular interventionalists, dubbed the "liberators" by Dr. Burks because of their unflappable advocacy for what has become known as the liberation procedure - the endovascular surgery designed to open the lesions causing the venous insufficiency, he said.
"Neurologists believe the interventionalists are overstating the possible value of CCSVI and that commercial interests are overriding scientific inquiry," according to Dr. Burks, a neurologist and clinical professor of medicine at the University of Nevada, Reno. Patients, armed with anecdotal evidence downloaded from the Internet, are certain that CCSVI surgery is the miracle they've been waiting for and perceive the hesitancy of U.S. and Canadian neurologists to embrace the treatment as evidence of a possible conspiracy with pharmaceutical companies who stand to lose billions of dollars if the surgery becomes a first-line treatment, he said. Further, he noted, advocates of CCSVI claim that neurologists who refuse patients' demands for diagnostic testing and surgical referral for CCSVI are jeopardizing the safety of those patients, who are traveling to foreign countries to get the care that they cannot receive in North America.
To date, the majority of the evidence regarding CCSVI diagnosis and treatment in MS is inconsistent, and can be confusing, Dr. Burks noted. In the initial study, Dr. Paolo Zamboni of the University of Ferrara in Italy, and colleagues, used Doppler ultrasound to examine venous drainage of the brain and spinal cord in 65 patients with different types of MS and 235 controls without MS and observed abnormal venous flow in all of the MS patients and none of the controls. The patterns of venous obstruction differed depending on MS stage and course, although there was no apparent relationship between disease severity and extent of venous obstruction, and MS treatment status did not influence the signs of CCSVI in any of the patients, the authors wrote (J. Neurol. Neurosurg. Psychiatry 2009;80:392-9).
The researchers went on to conduct an open pilot study to determine whether percutaneous transluminal angioplasty could safely and effectively treat the narrowing of the extracranial cerebrospinal veins in the 65 MS patients in which the condition was observed - 35 with relapsing-remitting MS, 20 with secondary progressive MS, and 10 with primary progressive MS. They reported significant improvements in MS clinical outcome measures, significant reductions in new brain lesions on MRI, and significant reductions in the number of relapses experienced by some of the patients.
The findings were limited, however, not only by the study design, but also by the fact that patients remained on their disease-modifying antirheumatic drug therapy during the study period and the timing and type of MRI scans varied among the patients, according to the authors. They also noted that restenosis of the internal jugular veins occurred in nearly half of the patients (J. Vasc. Surg. 2009;50:1348-58).
Since the initial paper, a number of CCSVI studies of various designs have been undertaken, with contradictory results. Following are some of the investigations reported within the past year:
P Researchers at the University of Buffalo found that up to 62% of the 280 patients with MS enrolled in the Combined Transcranial and Extracranial Venous Doppler Evaluation study - the first randomized clinical trial to evaluate MS patients for CCSVI - had the characteristic narrowing of the extracranial veins compared with approximately 22% of 220 healthy controls. While the results, which were reported at the annual meeting of the American Academy of Neurology, did not establish causation, they showed "that narrowing of the extracranial veins, at the very least, is an important association in multiple sclerosis," principal investigator Dr. Robert Zivadinov said in a statement. He acknowledged that the finding of vascular narrowing in nearly a quarter of the healthy controls warranted additional investigation (www.buffalo.edu/news/fast-execute.cgi/article-page.html?article=109370009).
P In an open-label study of extracranial Doppler criteria of CCSVI in 70 MS patients in Poland - 49 with relapsing-remitting MS, 5 with primary progressive MS, and 16 with secondary progressive MS - investigators detected at least two of four extracranial criteria in 90% of the patients. They concluded that, while the extracranial abnormalities could exist in various combinations, "the most common pathology in our patients was the presence of an inverted valve or another pathologic structure [like membranaceous or netlike septum] in the area of junction of the [internal jugular vein] with the brachiocephalic vein (Int. Angiol. 2010;29:109-14).
P A comparison of the internal jugular vein hemodynamics and morphology in 25 patients with MS and 25 controls identified abnormal findings in 92% of the MS patients and 24% of the controls, and evidence of CCSVI in 84% of the MS patients and none of the controls, leading the investigators to conclude that both hemodynamic abnormalities and morphologic changes in the internal jugular vein "are strongly associated with MS" (Int. Angiol. 2010;29:115-20).
P An extended extra- and transcranial color-coded sonography study in 56 MS patients and 20 controls detected no internal jugular vein stenosis and normal blood flow direction in all but 1 patient. There were no between-group differences in intracranial veins and during Valsalva maneuver, and none of the patients fulfilled more than one CCSVI criterion, according to the authors. They concluded that their findings "challenge the hypothesis that cerebral venous congestion plays a significant role in the pathogenesis of MS" (Ann. Neurol. 2010;68:173-83).
P Swedish investigators used phase-contrast MRI to study 21 relapsing-remitting MS patients and 20 healthy controls and found no differences in internal jugular venous outflow, aqueductal cerebrospinal fluid flow, or the presence of internal jugular blood reflux between the two groups. Although contrast-enhanced MR angiography showed internal jugular vein stenosis in 3 of the 21 MS patients, the authors stated they found no evidence "confirming the suggested vascular multiple sclerosis hypothesis" (Ann. Neurol. 2010;68:255-9).
P The authors of an MR venography and flow quantification study in The Netherlands compared the intracranial and extracranial venous anatomy and the intracerebral venous flow profiles of 20 MS patients and 20 age- and gender-matched controls, with image analysis performed by blinded interventional neuroradiologists. They identified venous system anomalies in 50% of the MS patients and 40% of the healthy controls and no venous backflow in either group. "Given the normal intracranial venous flow quantification results, it is likely that these findings reflect anatomical variants of venous drainage rather than clinically relevant venous outflow obstructions," the authors wrote (J. Neurol. Neurosurg. Psychiatry 2010 Oct. 27 [doi: 10.1136/jnnp.2010.223479]).
P Italian researchers investigating the occurrence of CCSVI in 50 consecutive patients with clinically isolated syndromes suggestive of MS reviewed the patients' extracranial and transcranial venous echo-color Doppler sonographs and compared the findings to those of 50 age- and gender-matched healthy controls as well as those of 60 patients with transient global amnesia (TGA) and 60 healthy controls matched to the TGA patients. They found extracranial Doppler sonographic abnormalities in 52% of patients with possible MS, 68.3% of patients with TGA, and 31.8% of the healthy controls. While eight of the patients with possible MS fulfilled the CCSVI criteria, selective phlebography showed no venous anomalies in seven of them. The authors concluded that there was no evidence of CCSVI at MS onset but recommended further studies to "clarify whether CCSVI is associated with later disease stages and characterizes the progressive forms of MS" (Ann. Neurol. 2011;69:90-9).
In a position statement, the Society of Interventional Radiology stated that at present, the published literature is "inconclusive on whether CCSVI is a clinically important factor and on whether balloon angioplasty and/or stent placement are effective in patients with MS" (J. Vasc. Interv. Radiol. 2010;21:1335-7).
Additionally, in a commentary on the treatment of CCSVI, representatives of the Cardiovascular and Interventional Radiological Society of Europe acknowledged that although several centers worldwide are promoting and performing balloon dilatation, with or without stenting for CCSVI, "We believe that until real scientific data are available for CCSVI and balloon dilatation, this treatment should not be offered to MS patients outside of a well designed clinical trial" (Cardiovasc. Intervent. Radiol. 2011;34:1-2).
Toward that end, the National Multiple Sclerosis Society of the United States and the MS Society of Canada have pledged $2.4 million in support of seven CCSVI research studies, including projects designed to evaluate venous abnormalities in children and teens with MS, patients with early and late stage MS, and those at risk for MS.
An international review panel comprising radiologists, vascular surgeons, and neurologists evaluated research applications via an expedited review process, according to the societies.
Dr. Burks disclosed relationships with various pharmaceutical companies. Dr. Baracchini had no relevant conflicts.
Rheumatoid Arthritis Confers Same Cardiovascular Risk as Diabetes
The cardiovascular risk in rheumatoid arthritis is comparable to that of diabetes, a large Danish study has shown.
Further, the risk of myocardial infarction (MI) in rheumatoid arthritis patients corresponds to that observed in the general population of individuals without the musculoskeletal condition who are, on average, 10 years older and does not appear to be affected by the duration of drug treatment for the disease, Dr. Jesper Lindhardsen of Gentofte University Hospital in Copenhagen, Denmark, and colleagues reported.
Using nationwide registers encompassing the entire Danish population older than 16 years, the investigators identified individuals with new-onset rheumatoid arthritis (RA), new onset diabetes, and new MI during a 10-year period, excluding individuals with prior disease and incomplete data entries from the full cohort of 4,311,022 subjects, they wrote.
During the 10-year study period, 9,921 individuals developed RA and 129,659 developed diabetes, the authors reported. Compared with the diabetes patients, "RA patients were more often women, used less cardioprotective medications, and had less comorbidity, whereas age was similar in the two groups," they reported.
Regarding cardiovascular outcomes, 265 of the RA patients and 3,948 of the diabetes patients had new MI, representing in both cohorts a 1.7 increased incidence rate ratio (IRR) of MI in a fully adjusted model compared with the general population in which 75,870 individuals had new myocardial infarctions, they wrote. The IRR among patients with both RA and diabetes was 2.6, "which roughly equaled the predicted additive risk for the two separate diseases, they wrote (Ann. Rheum. Dis. 2011;70:929-34).
The investigators conducted a nested case-control study that corroborated the comparable risk of MI in the RA and diabetes patients. The findings demonstrated that the increased risk in these groups was independent of treatment duration within the timeframe of the current study, they wrote.
Stratified by gender, the MI risk estimates did not differ between women and men in the RA group. In the diabetes patients, however, women were at significantly higher risk than men for the adverse cardiovascular outcome, the authors wrote. An age-dependent pattern of MI risk was also observed. Specifically, among women with RA and diabetes, respectively, the risk of MI in those younger than 50 years old was 5.5 and 5.9 times that observed in the age-matched reference group, they reported. Additionally, for women between 50 and 65 years of age, the IRRs were 1.7 and 2.6 for RA and diabetes patients, respectively.
The age-stratified patterns observed in men were different, the authors stated, noting that "the IRRs in the two oldest age groups were comparable, and even tended to be slightly higher in the 50-65 years age group of RA patients compared to the same-aged [diabetes] patients." And while the youngest men with RA had a markedly raised IRR, diabetes patients in the same age stratum had a significantly higher risk, with an IRR of 4.9 compared with 2.1, they said.
In a fully adjusted regression model in which the IRRs for MI in RA patients were calculated according to 10-year subject age intervals, "RA patients had the same, or higher, risk of MI as control subjects who were, on average, 10 years older," the authors reported.
Although the study has several limitations, including the identification of RA patients based on dispensed prescriptions and diagnosis versus the 1987 American College of Rheumatology criteria, the reliance on the use of glucose-lowering drugs as a proxy for diabetes, and the lack of information about classic cardiovascular risk factors, "the results corroborate and expand previous findings in this area of research and indicate that patients with RA should be considered for more aggressive primary [cardiovascular disease] prevention," the authors stressed.
In an accompanying editorial, Dr. Michael T. Nurmohamed and Dr. George Kitas of VU University Medical Centre in Amsterdam wrote that the findings of the current study should put to bed any doubt or debate about an enhanced cardiovascular risk in RA. "Importantly, they also provide further evidence that the cardiovascular risk in RA is broadly similar to that of contemporarily managed diabetes," they stated. The results of the study, as well as the success of cardiovascular risk management in diabetes provides a clear incentive to identify and actively manage, if necessary, cardiovascular risk in all RA patients as part of quality routine rheumatological practice" (Ann. Rheum. Dis. 2011;70:881-3).
The study was sponsored by an unrestricted grant from the Danish Rheumatism Association. The authors of the study and the accompanying editorial reported having no conflicts of interest to disclose.
The cardiovascular risk in rheumatoid arthritis is comparable to that of diabetes, a large Danish study has shown.
Further, the risk of myocardial infarction (MI) in rheumatoid arthritis patients corresponds to that observed in the general population of individuals without the musculoskeletal condition who are, on average, 10 years older and does not appear to be affected by the duration of drug treatment for the disease, Dr. Jesper Lindhardsen of Gentofte University Hospital in Copenhagen, Denmark, and colleagues reported.
Using nationwide registers encompassing the entire Danish population older than 16 years, the investigators identified individuals with new-onset rheumatoid arthritis (RA), new onset diabetes, and new MI during a 10-year period, excluding individuals with prior disease and incomplete data entries from the full cohort of 4,311,022 subjects, they wrote.
During the 10-year study period, 9,921 individuals developed RA and 129,659 developed diabetes, the authors reported. Compared with the diabetes patients, "RA patients were more often women, used less cardioprotective medications, and had less comorbidity, whereas age was similar in the two groups," they reported.
Regarding cardiovascular outcomes, 265 of the RA patients and 3,948 of the diabetes patients had new MI, representing in both cohorts a 1.7 increased incidence rate ratio (IRR) of MI in a fully adjusted model compared with the general population in which 75,870 individuals had new myocardial infarctions, they wrote. The IRR among patients with both RA and diabetes was 2.6, "which roughly equaled the predicted additive risk for the two separate diseases, they wrote (Ann. Rheum. Dis. 2011;70:929-34).
The investigators conducted a nested case-control study that corroborated the comparable risk of MI in the RA and diabetes patients. The findings demonstrated that the increased risk in these groups was independent of treatment duration within the timeframe of the current study, they wrote.
Stratified by gender, the MI risk estimates did not differ between women and men in the RA group. In the diabetes patients, however, women were at significantly higher risk than men for the adverse cardiovascular outcome, the authors wrote. An age-dependent pattern of MI risk was also observed. Specifically, among women with RA and diabetes, respectively, the risk of MI in those younger than 50 years old was 5.5 and 5.9 times that observed in the age-matched reference group, they reported. Additionally, for women between 50 and 65 years of age, the IRRs were 1.7 and 2.6 for RA and diabetes patients, respectively.
The age-stratified patterns observed in men were different, the authors stated, noting that "the IRRs in the two oldest age groups were comparable, and even tended to be slightly higher in the 50-65 years age group of RA patients compared to the same-aged [diabetes] patients." And while the youngest men with RA had a markedly raised IRR, diabetes patients in the same age stratum had a significantly higher risk, with an IRR of 4.9 compared with 2.1, they said.
In a fully adjusted regression model in which the IRRs for MI in RA patients were calculated according to 10-year subject age intervals, "RA patients had the same, or higher, risk of MI as control subjects who were, on average, 10 years older," the authors reported.
Although the study has several limitations, including the identification of RA patients based on dispensed prescriptions and diagnosis versus the 1987 American College of Rheumatology criteria, the reliance on the use of glucose-lowering drugs as a proxy for diabetes, and the lack of information about classic cardiovascular risk factors, "the results corroborate and expand previous findings in this area of research and indicate that patients with RA should be considered for more aggressive primary [cardiovascular disease] prevention," the authors stressed.
In an accompanying editorial, Dr. Michael T. Nurmohamed and Dr. George Kitas of VU University Medical Centre in Amsterdam wrote that the findings of the current study should put to bed any doubt or debate about an enhanced cardiovascular risk in RA. "Importantly, they also provide further evidence that the cardiovascular risk in RA is broadly similar to that of contemporarily managed diabetes," they stated. The results of the study, as well as the success of cardiovascular risk management in diabetes provides a clear incentive to identify and actively manage, if necessary, cardiovascular risk in all RA patients as part of quality routine rheumatological practice" (Ann. Rheum. Dis. 2011;70:881-3).
The study was sponsored by an unrestricted grant from the Danish Rheumatism Association. The authors of the study and the accompanying editorial reported having no conflicts of interest to disclose.
The cardiovascular risk in rheumatoid arthritis is comparable to that of diabetes, a large Danish study has shown.
Further, the risk of myocardial infarction (MI) in rheumatoid arthritis patients corresponds to that observed in the general population of individuals without the musculoskeletal condition who are, on average, 10 years older and does not appear to be affected by the duration of drug treatment for the disease, Dr. Jesper Lindhardsen of Gentofte University Hospital in Copenhagen, Denmark, and colleagues reported.
Using nationwide registers encompassing the entire Danish population older than 16 years, the investigators identified individuals with new-onset rheumatoid arthritis (RA), new onset diabetes, and new MI during a 10-year period, excluding individuals with prior disease and incomplete data entries from the full cohort of 4,311,022 subjects, they wrote.
During the 10-year study period, 9,921 individuals developed RA and 129,659 developed diabetes, the authors reported. Compared with the diabetes patients, "RA patients were more often women, used less cardioprotective medications, and had less comorbidity, whereas age was similar in the two groups," they reported.
Regarding cardiovascular outcomes, 265 of the RA patients and 3,948 of the diabetes patients had new MI, representing in both cohorts a 1.7 increased incidence rate ratio (IRR) of MI in a fully adjusted model compared with the general population in which 75,870 individuals had new myocardial infarctions, they wrote. The IRR among patients with both RA and diabetes was 2.6, "which roughly equaled the predicted additive risk for the two separate diseases, they wrote (Ann. Rheum. Dis. 2011;70:929-34).
The investigators conducted a nested case-control study that corroborated the comparable risk of MI in the RA and diabetes patients. The findings demonstrated that the increased risk in these groups was independent of treatment duration within the timeframe of the current study, they wrote.
Stratified by gender, the MI risk estimates did not differ between women and men in the RA group. In the diabetes patients, however, women were at significantly higher risk than men for the adverse cardiovascular outcome, the authors wrote. An age-dependent pattern of MI risk was also observed. Specifically, among women with RA and diabetes, respectively, the risk of MI in those younger than 50 years old was 5.5 and 5.9 times that observed in the age-matched reference group, they reported. Additionally, for women between 50 and 65 years of age, the IRRs were 1.7 and 2.6 for RA and diabetes patients, respectively.
The age-stratified patterns observed in men were different, the authors stated, noting that "the IRRs in the two oldest age groups were comparable, and even tended to be slightly higher in the 50-65 years age group of RA patients compared to the same-aged [diabetes] patients." And while the youngest men with RA had a markedly raised IRR, diabetes patients in the same age stratum had a significantly higher risk, with an IRR of 4.9 compared with 2.1, they said.
In a fully adjusted regression model in which the IRRs for MI in RA patients were calculated according to 10-year subject age intervals, "RA patients had the same, or higher, risk of MI as control subjects who were, on average, 10 years older," the authors reported.
Although the study has several limitations, including the identification of RA patients based on dispensed prescriptions and diagnosis versus the 1987 American College of Rheumatology criteria, the reliance on the use of glucose-lowering drugs as a proxy for diabetes, and the lack of information about classic cardiovascular risk factors, "the results corroborate and expand previous findings in this area of research and indicate that patients with RA should be considered for more aggressive primary [cardiovascular disease] prevention," the authors stressed.
In an accompanying editorial, Dr. Michael T. Nurmohamed and Dr. George Kitas of VU University Medical Centre in Amsterdam wrote that the findings of the current study should put to bed any doubt or debate about an enhanced cardiovascular risk in RA. "Importantly, they also provide further evidence that the cardiovascular risk in RA is broadly similar to that of contemporarily managed diabetes," they stated. The results of the study, as well as the success of cardiovascular risk management in diabetes provides a clear incentive to identify and actively manage, if necessary, cardiovascular risk in all RA patients as part of quality routine rheumatological practice" (Ann. Rheum. Dis. 2011;70:881-3).
The study was sponsored by an unrestricted grant from the Danish Rheumatism Association. The authors of the study and the accompanying editorial reported having no conflicts of interest to disclose.
FROM ANNALS OF THE RHEUMATIC DISEASE
Major Finding: Rheumatoid arthritis is associated with the same risk of myocardial infarction as diabetes mellitus.
Data Source: A large, population-based study of the incidence of new-onset rheumatoid arthritis, diabetes, and myocardial infarction using Danish patient registry information covering a 10 year period.
Disclosures: The study was supported by an unrestricted grant from the Danish Rheumatism Association. The authors disclosed having no conflicts of interest.