Erik J. Lindbloom, MD, MSPH

ABSTRACT

BACKGROUND: One of the proposed benefits of postmenopausal hormone replacement therapy (HRT) is the prevention of coronary heart disease. This proposal is based on evidence from nonrandomized observational studies and intermediate outcomes such as improved lipid profiles. The possibility of harm from HRT has also been reported, particularly regarding breast cancer and thromboembolic disease. The Heart and Estrogen/progestin Replacement Study recently challenged the benefits of HRT, showing no overall protective effect on coronary heart disease (and an increased risk of harm in the first year of treatment) for women with prior coronary heart disease.

POPULATION STUDIED: The Women’s Health Initiative is a set of clinical trials with more than 160,000 women enrolled in studies of low-fat diet, calcium and vitamin D supplementation, and post-menopausal hormone use. This particular report focused on the trial of estrogen plus progestin in women with an intact uterus. A total of 16,608 post-menopausal women were randomized to receive either 1 daily tablet of conjugated equine estrogen 0.625 mg and medroxyprogesterone acetate 2.5 mg (Prempro) or placebo. Women were excluded if they had a history of breast cancer, other cancer within 10 years, hysterectomy, anemia, thrombocytopenia, alcoholism, or dementia. Ages ranged from 50 to 79 years (mean 63 years). Approximately 36% of the women were being treated for hypertension, 4.4% had diabetes, and 7.7% reported a history of cardiovascular disease.

STUDY DESIGN AND VALIDITY: This was a well-designed double-blind, randomized controlled trial with concealed allocation. Baseline characteristics were similar between groups. Follow-up was conducted 6 weeks after randomization, every 6 months with questionnaires, and annually with in-clinic visits. Intention-to-treat analysis was appropriate and would tend to find smaller differences between groups given the high dropout rates (42% in the HRT group and 38% in the placebo group). The trial was originally designed to last more than 8 years, but the independent safety monitoring board recommended stopping the trial when the difference in breast cancer rates exceeded a predetermined threshold and the global index was supportive of harm. When the trial was stopped in the spring of 2002, the average follow-up period was 5.2 years.

OUTCOMES MEASURED: The primary outcome measure was the rate of coronary heart disease, defined as acute myocardial infarction requiring overnight hospitalization, silent myocardial infarction determined from serial electrocardiograms, or coronary heart disease death. The secondary outcome measure was hip fracture rate. The primary adverse outcome measure was invasive breast cancer rate. Reported outcomes also included other cancers, total fractures, stroke, pulmonary embolism, deep vein thrombosis, and total mortality. A global index of outcomes was also calculated as a summary measure of risks and benefits. No measures of vasomotor symptoms or quality of life were reported.

RESULTS: Women in the HRT group had a higher annual incidence of coronary heart disease (0.37% vs 0.30%, NNH = 1429), invasive breast cancer (0.38% vs 0.30%, NNH = 1250), stroke (0.29% vs 0.21%, NNH = 1250), and venous thromboembolic disease (0.34% vs 0.16%, NNH = 556). Bone fractures were less prevalent in the HRT group (total annual fracture rate, 1.47% vs 1.91%, NNT = 228), as was colorectal cancer (0.10% vs 0.16%, NNT = 1667). All of these differences except thromboembolic disease lost statistical significance when adjusting for multiple comparisons, but subgroup analyses showed these differences in adverse events regardless of baseline risks of coronary heart disease and breast cancer. Individuals who adhered to the study medication showed greater differences in adverse events, and individuals who had already used HRT before the study had higher rates of breast cancer. Overall mortality was not different in the 2 groups. The excess risk of events in the global index was 19 per 10,000 person-years. In other words, an average of 1 additional adverse event would be expected over 5 years of treatment for every 100 women meeting these criteria.

ABSTRACT

BACKGROUND: One of the proposed benefits of postmenopausal hormone replacement therapy (HRT) is the prevention of coronary heart disease. This proposal is based on evidence from nonrandomized observational studies and intermediate outcomes such as improved lipid profiles. The possibility of harm from HRT has also been reported, particularly regarding breast cancer and thromboembolic disease. The Heart and Estrogen/progestin Replacement Study recently challenged the benefits of HRT, showing no overall protective effect on coronary heart disease (and an increased risk of harm in the first year of treatment) for women with prior coronary heart disease.

POPULATION STUDIED: The Women’s Health Initiative is a set of clinical trials with more than 160,000 women enrolled in studies of low-fat diet, calcium and vitamin D supplementation, and post-menopausal hormone use. This particular report focused on the trial of estrogen plus progestin in women with an intact uterus. A total of 16,608 post-menopausal women were randomized to receive either 1 daily tablet of conjugated equine estrogen 0.625 mg and medroxyprogesterone acetate 2.5 mg (Prempro) or placebo. Women were excluded if they had a history of breast cancer, other cancer within 10 years, hysterectomy, anemia, thrombocytopenia, alcoholism, or dementia. Ages ranged from 50 to 79 years (mean 63 years). Approximately 36% of the women were being treated for hypertension, 4.4% had diabetes, and 7.7% reported a history of cardiovascular disease.

STUDY DESIGN AND VALIDITY: This was a well-designed double-blind, randomized controlled trial with concealed allocation. Baseline characteristics were similar between groups. Follow-up was conducted 6 weeks after randomization, every 6 months with questionnaires, and annually with in-clinic visits. Intention-to-treat analysis was appropriate and would tend to find smaller differences between groups given the high dropout rates (42% in the HRT group and 38% in the placebo group). The trial was originally designed to last more than 8 years, but the independent safety monitoring board recommended stopping the trial when the difference in breast cancer rates exceeded a predetermined threshold and the global index was supportive of harm. When the trial was stopped in the spring of 2002, the average follow-up period was 5.2 years.

OUTCOMES MEASURED: The primary outcome measure was the rate of coronary heart disease, defined as acute myocardial infarction requiring overnight hospitalization, silent myocardial infarction determined from serial electrocardiograms, or coronary heart disease death. The secondary outcome measure was hip fracture rate. The primary adverse outcome measure was invasive breast cancer rate. Reported outcomes also included other cancers, total fractures, stroke, pulmonary embolism, deep vein thrombosis, and total mortality. A global index of outcomes was also calculated as a summary measure of risks and benefits. No measures of vasomotor symptoms or quality of life were reported.

RESULTS: Women in the HRT group had a higher annual incidence of coronary heart disease (0.37% vs 0.30%, NNH = 1429), invasive breast cancer (0.38% vs 0.30%, NNH = 1250), stroke (0.29% vs 0.21%, NNH = 1250), and venous thromboembolic disease (0.34% vs 0.16%, NNH = 556). Bone fractures were less prevalent in the HRT group (total annual fracture rate, 1.47% vs 1.91%, NNT = 228), as was colorectal cancer (0.10% vs 0.16%, NNT = 1667). All of these differences except thromboembolic disease lost statistical significance when adjusting for multiple comparisons, but subgroup analyses showed these differences in adverse events regardless of baseline risks of coronary heart disease and breast cancer. Individuals who adhered to the study medication showed greater differences in adverse events, and individuals who had already used HRT before the study had higher rates of breast cancer. Overall mortality was not different in the 2 groups. The excess risk of events in the global index was 19 per 10,000 person-years. In other words, an average of 1 additional adverse event would be expected over 5 years of treatment for every 100 women meeting these criteria.

ABSTRACT

BACKGROUND: One of the proposed benefits of postmenopausal hormone replacement therapy (HRT) is the prevention of coronary heart disease. This proposal is based on evidence from nonrandomized observational studies and intermediate outcomes such as improved lipid profiles. The possibility of harm from HRT has also been reported, particularly regarding breast cancer and thromboembolic disease. The Heart and Estrogen/progestin Replacement Study recently challenged the benefits of HRT, showing no overall protective effect on coronary heart disease (and an increased risk of harm in the first year of treatment) for women with prior coronary heart disease.

POPULATION STUDIED: The Women’s Health Initiative is a set of clinical trials with more than 160,000 women enrolled in studies of low-fat diet, calcium and vitamin D supplementation, and post-menopausal hormone use. This particular report focused on the trial of estrogen plus progestin in women with an intact uterus. A total of 16,608 post-menopausal women were randomized to receive either 1 daily tablet of conjugated equine estrogen 0.625 mg and medroxyprogesterone acetate 2.5 mg (Prempro) or placebo. Women were excluded if they had a history of breast cancer, other cancer within 10 years, hysterectomy, anemia, thrombocytopenia, alcoholism, or dementia. Ages ranged from 50 to 79 years (mean 63 years). Approximately 36% of the women were being treated for hypertension, 4.4% had diabetes, and 7.7% reported a history of cardiovascular disease.

STUDY DESIGN AND VALIDITY: This was a well-designed double-blind, randomized controlled trial with concealed allocation. Baseline characteristics were similar between groups. Follow-up was conducted 6 weeks after randomization, every 6 months with questionnaires, and annually with in-clinic visits. Intention-to-treat analysis was appropriate and would tend to find smaller differences between groups given the high dropout rates (42% in the HRT group and 38% in the placebo group). The trial was originally designed to last more than 8 years, but the independent safety monitoring board recommended stopping the trial when the difference in breast cancer rates exceeded a predetermined threshold and the global index was supportive of harm. When the trial was stopped in the spring of 2002, the average follow-up period was 5.2 years.

OUTCOMES MEASURED: The primary outcome measure was the rate of coronary heart disease, defined as acute myocardial infarction requiring overnight hospitalization, silent myocardial infarction determined from serial electrocardiograms, or coronary heart disease death. The secondary outcome measure was hip fracture rate. The primary adverse outcome measure was invasive breast cancer rate. Reported outcomes also included other cancers, total fractures, stroke, pulmonary embolism, deep vein thrombosis, and total mortality. A global index of outcomes was also calculated as a summary measure of risks and benefits. No measures of vasomotor symptoms or quality of life were reported.

RESULTS: Women in the HRT group had a higher annual incidence of coronary heart disease (0.37% vs 0.30%, NNH = 1429), invasive breast cancer (0.38% vs 0.30%, NNH = 1250), stroke (0.29% vs 0.21%, NNH = 1250), and venous thromboembolic disease (0.34% vs 0.16%, NNH = 556). Bone fractures were less prevalent in the HRT group (total annual fracture rate, 1.47% vs 1.91%, NNT = 228), as was colorectal cancer (0.10% vs 0.16%, NNT = 1667). All of these differences except thromboembolic disease lost statistical significance when adjusting for multiple comparisons, but subgroup analyses showed these differences in adverse events regardless of baseline risks of coronary heart disease and breast cancer. Individuals who adhered to the study medication showed greater differences in adverse events, and individuals who had already used HRT before the study had higher rates of breast cancer. Overall mortality was not different in the 2 groups. The excess risk of events in the global index was 19 per 10,000 person-years. In other words, an average of 1 additional adverse event would be expected over 5 years of treatment for every 100 women meeting these criteria.

ABSTRACT

BACKGROUND: Clopidogrel is a platelet aggregation inhibitor that is slightly more effective than aspirin in reducing the risk of cardiovascular events in individuals with preexisting cardiovascular disease (0.51% annual absolute risk reduction; Lancet 1996; 348:1329–39). However, clopidogrel is currently 80 times more expensive than aspirin. The authors looked at the risks, benefits, and costs of long-term use of various therapeutic strategies involving these 2 medications.
POPULATION STUDIED: A computer simulation, known as the Coronary Heart Disease Policy Model, was used to predict the number of patients in the United States (35–84 years) who would develop coronary disease before or during the next 25 years, as well as the number of subsequent cardiovascular events and deaths these individuals would experience. Only patients predicted to survive their first month after a cardiac event were included in the therapeutic intervention analysis. Parameters for the model were based on cohort studies and clinical trials found in the medical literature.
STUDY DESIGN AND VALIDITY: Beginning with their estimated number of Americans with coronary disease and cardiovascular events, the authors predicted the reduction in events using aspirin, clopidogrel, or both. The 4 possible treatment strategies were (1) aspirin 325 mg/day for all eligible patients; (2) aspirin for all eligible patients or clopidogrel 75 mg/day for the remaining 5.7% ineligible for aspirin; (3) clopidogrel 75 mg/day for all patients; or (4) a combination of clopidogrel for all patients plus aspirin for all eligible patients. They also considered costs of various interventions, including hospitalizations, rehabilitation services, outpatient and home services, and treatment for adverse drug effects such as gastrointestinal bleeding. To carry out the cost-effectiveness analysis over such a long time period, the authors discounted costs at a rate of 3% per year (a typical amount) and converted all values to year-2000 US dollars. Sensitivity analysis used upper and lower bounds of reductions from past trial data to give a reasonable range of values. As with all hypothetical cost-effectiveness studies, this study only represents the authors’ best estimates of costs and benefits, not actual results from a therapeutic trial or cohort. Issues such as the safety of combination therapy over this prolonged time period have not been well established.
OUTCOMES MEASURED: The main outcome was the cost per quality-adjusted life year (QALY) gained, that is, the cost of an additional year of optimal health.
RESULTS: Aspirin alone in all eligible patients (strategy #1) resulted in an estimated $11,000 per QALY gained. Giving clopidogrel to the 5.7% of patients ineligible for aspirin (strategy #2) would prevent some subsequent events at an increased cost, resulting in a total estimate of $31,000 per QALY gained compared with the first strategy. Using clopidogrel alone for everyone (strategy #3) led to a very high estimated cost of $250,000 per QALY gained compared with strategy #2. Combination therapy of clopidogrel for everyone plus aspirin for the 96.3% of eligible patients (strategy #4) resulted in an estimated cost of $130,000 per QALY gained compared with strategy #2. However, in patients with annual risks 3 times as high as that of the average patient with coronary disease, this ratio fell below $64,000 per QALY gained.

ABSTRACT

BACKGROUND: Clopidogrel is a platelet aggregation inhibitor that is slightly more effective than aspirin in reducing the risk of cardiovascular events in individuals with preexisting cardiovascular disease (0.51% annual absolute risk reduction; Lancet 1996; 348:1329–39). However, clopidogrel is currently 80 times more expensive than aspirin. The authors looked at the risks, benefits, and costs of long-term use of various therapeutic strategies involving these 2 medications.
POPULATION STUDIED: A computer simulation, known as the Coronary Heart Disease Policy Model, was used to predict the number of patients in the United States (35–84 years) who would develop coronary disease before or during the next 25 years, as well as the number of subsequent cardiovascular events and deaths these individuals would experience. Only patients predicted to survive their first month after a cardiac event were included in the therapeutic intervention analysis. Parameters for the model were based on cohort studies and clinical trials found in the medical literature.
STUDY DESIGN AND VALIDITY: Beginning with their estimated number of Americans with coronary disease and cardiovascular events, the authors predicted the reduction in events using aspirin, clopidogrel, or both. The 4 possible treatment strategies were (1) aspirin 325 mg/day for all eligible patients; (2) aspirin for all eligible patients or clopidogrel 75 mg/day for the remaining 5.7% ineligible for aspirin; (3) clopidogrel 75 mg/day for all patients; or (4) a combination of clopidogrel for all patients plus aspirin for all eligible patients. They also considered costs of various interventions, including hospitalizations, rehabilitation services, outpatient and home services, and treatment for adverse drug effects such as gastrointestinal bleeding. To carry out the cost-effectiveness analysis over such a long time period, the authors discounted costs at a rate of 3% per year (a typical amount) and converted all values to year-2000 US dollars. Sensitivity analysis used upper and lower bounds of reductions from past trial data to give a reasonable range of values. As with all hypothetical cost-effectiveness studies, this study only represents the authors’ best estimates of costs and benefits, not actual results from a therapeutic trial or cohort. Issues such as the safety of combination therapy over this prolonged time period have not been well established.
OUTCOMES MEASURED: The main outcome was the cost per quality-adjusted life year (QALY) gained, that is, the cost of an additional year of optimal health.
RESULTS: Aspirin alone in all eligible patients (strategy #1) resulted in an estimated $11,000 per QALY gained. Giving clopidogrel to the 5.7% of patients ineligible for aspirin (strategy #2) would prevent some subsequent events at an increased cost, resulting in a total estimate of $31,000 per QALY gained compared with the first strategy. Using clopidogrel alone for everyone (strategy #3) led to a very high estimated cost of $250,000 per QALY gained compared with strategy #2. Combination therapy of clopidogrel for everyone plus aspirin for the 96.3% of eligible patients (strategy #4) resulted in an estimated cost of $130,000 per QALY gained compared with strategy #2. However, in patients with annual risks 3 times as high as that of the average patient with coronary disease, this ratio fell below $64,000 per QALY gained.

ABSTRACT

BACKGROUND: Clopidogrel is a platelet aggregation inhibitor that is slightly more effective than aspirin in reducing the risk of cardiovascular events in individuals with preexisting cardiovascular disease (0.51% annual absolute risk reduction; Lancet 1996; 348:1329–39). However, clopidogrel is currently 80 times more expensive than aspirin. The authors looked at the risks, benefits, and costs of long-term use of various therapeutic strategies involving these 2 medications.
POPULATION STUDIED: A computer simulation, known as the Coronary Heart Disease Policy Model, was used to predict the number of patients in the United States (35–84 years) who would develop coronary disease before or during the next 25 years, as well as the number of subsequent cardiovascular events and deaths these individuals would experience. Only patients predicted to survive their first month after a cardiac event were included in the therapeutic intervention analysis. Parameters for the model were based on cohort studies and clinical trials found in the medical literature.
STUDY DESIGN AND VALIDITY: Beginning with their estimated number of Americans with coronary disease and cardiovascular events, the authors predicted the reduction in events using aspirin, clopidogrel, or both. The 4 possible treatment strategies were (1) aspirin 325 mg/day for all eligible patients; (2) aspirin for all eligible patients or clopidogrel 75 mg/day for the remaining 5.7% ineligible for aspirin; (3) clopidogrel 75 mg/day for all patients; or (4) a combination of clopidogrel for all patients plus aspirin for all eligible patients. They also considered costs of various interventions, including hospitalizations, rehabilitation services, outpatient and home services, and treatment for adverse drug effects such as gastrointestinal bleeding. To carry out the cost-effectiveness analysis over such a long time period, the authors discounted costs at a rate of 3% per year (a typical amount) and converted all values to year-2000 US dollars. Sensitivity analysis used upper and lower bounds of reductions from past trial data to give a reasonable range of values. As with all hypothetical cost-effectiveness studies, this study only represents the authors’ best estimates of costs and benefits, not actual results from a therapeutic trial or cohort. Issues such as the safety of combination therapy over this prolonged time period have not been well established.
OUTCOMES MEASURED: The main outcome was the cost per quality-adjusted life year (QALY) gained, that is, the cost of an additional year of optimal health.
RESULTS: Aspirin alone in all eligible patients (strategy #1) resulted in an estimated $11,000 per QALY gained. Giving clopidogrel to the 5.7% of patients ineligible for aspirin (strategy #2) would prevent some subsequent events at an increased cost, resulting in a total estimate of $31,000 per QALY gained compared with the first strategy. Using clopidogrel alone for everyone (strategy #3) led to a very high estimated cost of $250,000 per QALY gained compared with strategy #2. Combination therapy of clopidogrel for everyone plus aspirin for the 96.3% of eligible patients (strategy #4) resulted in an estimated cost of $130,000 per QALY gained compared with strategy #2. However, in patients with annual risks 3 times as high as that of the average patient with coronary disease, this ratio fell below $64,000 per QALY gained.

Evidence summary

Aortic stenosis is a narrowing of the aortic valve. Degree of severity is judged by valve area: mild (1.5–2.0 cm²), moderate (1.0–1.5 cm²), severe (< 1.0 cm²). Alternatively, stenosis may be classified by transvalvular gradient or jet velocity, the latter being the easier quantity to measure by echocardiogram. Prevalence of aortic stenosis increases with age; one series of 1243 elderly women (mean age of 82) found mild stenosis in 10%, moderate stenosis in 6%, and severe stenosis in 2%.¹ Natural history studies show that once classic symptoms develop, average survival decreases to 5 years with the onset of angina, 3 years after cardiac syncope, and 2 years after heart failure.² The incidence of sudden death increases from < 1% annually among asymptomatic patients to 15% to 20% among symptomatic patients.^3,4

Aortic stenosis is suggested by such findings as a harsh systolic murmur at the right upper sternal border, pulsus parvus et tardus, and a sustained point of maximal impulse. Exercise stress testing may provide additional information. In one prospective study of 123 patients, those who had a greater increase in valve area, cardiac output, and blood pressure and a smaller decrease in stroke volume on stress echocardiogram were more likely to remain asymptomatic for the entire length of their time in the study, an average of 2.5 years.⁵

Asymptomatic patients with aortic stenosis who undergo coronary artery bypass grafting (CABG) often have their aortic valve replaced at the same time; the timing of aortic valve replacement in patients not requiring CABG is controversial. One prospective study found the severity of stenosis at baseline to be the strongest prognostic predictor. Patients with a jet velocity of < 3.0 m/s were unlikely to develop symptoms within 5 years; those with a jet velocity of 4.0 m/s had a > 50% likelihood of developing symptoms or dying within 2 years.⁵ Another study followed 128 patients for 4 years and found that moderate to severe valvular calcification and an increase in jet velocity of 0.3 m/s/year were the best prognostic predictors.⁶ Almost 80% of those with both calcification and a rapid change in jet velocity underwent surgery or died within 2 years⁶ (Table).

TABLE
Indications for possible valve replacement with asymptomatic aortic stenosis

Recommendations from others

The American College of Cardiology/American Heart Association Task Force on Practice Guidelines recommends echocardiograms every 5 years for mild stenosis, every 2 years for moderate stenosis, and annually for severe stenosis.⁴ There is no guideline for exercise testing. Aortic valve replacement is recommended for symptomatic patients and patients with severe stenosis undergoing CABG or other valvular or aortic surgery.

Clinical Commentary by Ken Grauer, MD; and search strategy, at www.fpin.org.

Evidence summary

Aortic stenosis is a narrowing of the aortic valve. Degree of severity is judged by valve area: mild (1.5–2.0 cm²), moderate (1.0–1.5 cm²), severe (< 1.0 cm²). Alternatively, stenosis may be classified by transvalvular gradient or jet velocity, the latter being the easier quantity to measure by echocardiogram. Prevalence of aortic stenosis increases with age; one series of 1243 elderly women (mean age of 82) found mild stenosis in 10%, moderate stenosis in 6%, and severe stenosis in 2%.¹ Natural history studies show that once classic symptoms develop, average survival decreases to 5 years with the onset of angina, 3 years after cardiac syncope, and 2 years after heart failure.² The incidence of sudden death increases from < 1% annually among asymptomatic patients to 15% to 20% among symptomatic patients.^3,4

Aortic stenosis is suggested by such findings as a harsh systolic murmur at the right upper sternal border, pulsus parvus et tardus, and a sustained point of maximal impulse. Exercise stress testing may provide additional information. In one prospective study of 123 patients, those who had a greater increase in valve area, cardiac output, and blood pressure and a smaller decrease in stroke volume on stress echocardiogram were more likely to remain asymptomatic for the entire length of their time in the study, an average of 2.5 years.⁵

Asymptomatic patients with aortic stenosis who undergo coronary artery bypass grafting (CABG) often have their aortic valve replaced at the same time; the timing of aortic valve replacement in patients not requiring CABG is controversial. One prospective study found the severity of stenosis at baseline to be the strongest prognostic predictor. Patients with a jet velocity of < 3.0 m/s were unlikely to develop symptoms within 5 years; those with a jet velocity of 4.0 m/s had a > 50% likelihood of developing symptoms or dying within 2 years.⁵ Another study followed 128 patients for 4 years and found that moderate to severe valvular calcification and an increase in jet velocity of 0.3 m/s/year were the best prognostic predictors.⁶ Almost 80% of those with both calcification and a rapid change in jet velocity underwent surgery or died within 2 years⁶ (Table).

TABLE
Indications for possible valve replacement with asymptomatic aortic stenosis

Recommendations from others

The American College of Cardiology/American Heart Association Task Force on Practice Guidelines recommends echocardiograms every 5 years for mild stenosis, every 2 years for moderate stenosis, and annually for severe stenosis.⁴ There is no guideline for exercise testing. Aortic valve replacement is recommended for symptomatic patients and patients with severe stenosis undergoing CABG or other valvular or aortic surgery.

Clinical Commentary by Ken Grauer, MD; and search strategy, at www.fpin.org.

Evidence summary

Aortic stenosis is a narrowing of the aortic valve. Degree of severity is judged by valve area: mild (1.5–2.0 cm²), moderate (1.0–1.5 cm²), severe (< 1.0 cm²). Alternatively, stenosis may be classified by transvalvular gradient or jet velocity, the latter being the easier quantity to measure by echocardiogram. Prevalence of aortic stenosis increases with age; one series of 1243 elderly women (mean age of 82) found mild stenosis in 10%, moderate stenosis in 6%, and severe stenosis in 2%.¹ Natural history studies show that once classic symptoms develop, average survival decreases to 5 years with the onset of angina, 3 years after cardiac syncope, and 2 years after heart failure.² The incidence of sudden death increases from < 1% annually among asymptomatic patients to 15% to 20% among symptomatic patients.^3,4

Aortic stenosis is suggested by such findings as a harsh systolic murmur at the right upper sternal border, pulsus parvus et tardus, and a sustained point of maximal impulse. Exercise stress testing may provide additional information. In one prospective study of 123 patients, those who had a greater increase in valve area, cardiac output, and blood pressure and a smaller decrease in stroke volume on stress echocardiogram were more likely to remain asymptomatic for the entire length of their time in the study, an average of 2.5 years.⁵

Asymptomatic patients with aortic stenosis who undergo coronary artery bypass grafting (CABG) often have their aortic valve replaced at the same time; the timing of aortic valve replacement in patients not requiring CABG is controversial. One prospective study found the severity of stenosis at baseline to be the strongest prognostic predictor. Patients with a jet velocity of < 3.0 m/s were unlikely to develop symptoms within 5 years; those with a jet velocity of 4.0 m/s had a > 50% likelihood of developing symptoms or dying within 2 years.⁵ Another study followed 128 patients for 4 years and found that moderate to severe valvular calcification and an increase in jet velocity of 0.3 m/s/year were the best prognostic predictors.⁶ Almost 80% of those with both calcification and a rapid change in jet velocity underwent surgery or died within 2 years⁶ (Table).

TABLE
Indications for possible valve replacement with asymptomatic aortic stenosis

Recommendations from others

The American College of Cardiology/American Heart Association Task Force on Practice Guidelines recommends echocardiograms every 5 years for mild stenosis, every 2 years for moderate stenosis, and annually for severe stenosis.⁴ There is no guideline for exercise testing. Aortic valve replacement is recommended for symptomatic patients and patients with severe stenosis undergoing CABG or other valvular or aortic surgery.

Clinical Commentary by Ken Grauer, MD; and search strategy, at www.fpin.org.

ABSTRACT

BACKGROUND: Current use of cervical spine (C-spine) radiography for alert and stable trauma patients is highly variable and expensive in practice. A recent clinical decision rule to identify low-risk patients was accurate in distinguishing those who would not need radiography (high sensitivity) but would result in many patients being unnecessarily imaged (low specificity).¹ The originators of the Ottawa Ankle and Knee rules have created a decision rule for use of C-spine radiography.

POPULATION STUDIED: The study enrolled patients 16 years and older who sustained acute blunt trauma to the head or neck and presented to an emergency department (ED) of 10 large Canadian hospitals. Patients had to be completely alert with normal vital signs. They either had to report neck pain or be nonambulatory with visible injury above the clavicles after a dangerous mechanism of injury. Patients were not studied if they were injured more than 48 hours before presentation, were returning for reassessment of the same injury, were pregnant, or had penetrating trauma, acute paralysis, or known vertebral disease.

STUDY DESIGN AND VALIDITY: This was a prospective cohort study in which physicians determined 20 standardized clinical findings from the history and physical examination. The physician would then decide whether to obtain C-spine radiography; if no X-ray was obtained, a structured telephone interview 14 days later determined whether a clinically important C-spine injury had taken place. Clinical findings were then analyzed for their association with significant C-spine injuries. Although the study attempted to enroll consecutive patients, 3281 of 12,782 eligible patients were not enrolled for unclear reasons, and 577 patients could not be contacted by telephone for follow-up.

OUTCOMES MEASURED: The primary outcome measure was clinically important C-spine injury, defined as a fracture, dislocation, or ligamentous instability demonstrated by diagnostic imaging.

RESULTS: Approximately 69% of patients underwent C-spine radiography, and 31% underwent the 14-day follow-up phone interview. A total of 151 (1.7%) were determined to have a clinically important C-spine injury. No patients who did not undergo radiography were found to have important injuries 14 days later.

ABSTRACT

BACKGROUND: Current use of cervical spine (C-spine) radiography for alert and stable trauma patients is highly variable and expensive in practice. A recent clinical decision rule to identify low-risk patients was accurate in distinguishing those who would not need radiography (high sensitivity) but would result in many patients being unnecessarily imaged (low specificity).¹ The originators of the Ottawa Ankle and Knee rules have created a decision rule for use of C-spine radiography.

POPULATION STUDIED: The study enrolled patients 16 years and older who sustained acute blunt trauma to the head or neck and presented to an emergency department (ED) of 10 large Canadian hospitals. Patients had to be completely alert with normal vital signs. They either had to report neck pain or be nonambulatory with visible injury above the clavicles after a dangerous mechanism of injury. Patients were not studied if they were injured more than 48 hours before presentation, were returning for reassessment of the same injury, were pregnant, or had penetrating trauma, acute paralysis, or known vertebral disease.

STUDY DESIGN AND VALIDITY: This was a prospective cohort study in which physicians determined 20 standardized clinical findings from the history and physical examination. The physician would then decide whether to obtain C-spine radiography; if no X-ray was obtained, a structured telephone interview 14 days later determined whether a clinically important C-spine injury had taken place. Clinical findings were then analyzed for their association with significant C-spine injuries. Although the study attempted to enroll consecutive patients, 3281 of 12,782 eligible patients were not enrolled for unclear reasons, and 577 patients could not be contacted by telephone for follow-up.

OUTCOMES MEASURED: The primary outcome measure was clinically important C-spine injury, defined as a fracture, dislocation, or ligamentous instability demonstrated by diagnostic imaging.

RESULTS: Approximately 69% of patients underwent C-spine radiography, and 31% underwent the 14-day follow-up phone interview. A total of 151 (1.7%) were determined to have a clinically important C-spine injury. No patients who did not undergo radiography were found to have important injuries 14 days later.

ABSTRACT

BACKGROUND: Current use of cervical spine (C-spine) radiography for alert and stable trauma patients is highly variable and expensive in practice. A recent clinical decision rule to identify low-risk patients was accurate in distinguishing those who would not need radiography (high sensitivity) but would result in many patients being unnecessarily imaged (low specificity).¹ The originators of the Ottawa Ankle and Knee rules have created a decision rule for use of C-spine radiography.

POPULATION STUDIED: The study enrolled patients 16 years and older who sustained acute blunt trauma to the head or neck and presented to an emergency department (ED) of 10 large Canadian hospitals. Patients had to be completely alert with normal vital signs. They either had to report neck pain or be nonambulatory with visible injury above the clavicles after a dangerous mechanism of injury. Patients were not studied if they were injured more than 48 hours before presentation, were returning for reassessment of the same injury, were pregnant, or had penetrating trauma, acute paralysis, or known vertebral disease.

STUDY DESIGN AND VALIDITY: This was a prospective cohort study in which physicians determined 20 standardized clinical findings from the history and physical examination. The physician would then decide whether to obtain C-spine radiography; if no X-ray was obtained, a structured telephone interview 14 days later determined whether a clinically important C-spine injury had taken place. Clinical findings were then analyzed for their association with significant C-spine injuries. Although the study attempted to enroll consecutive patients, 3281 of 12,782 eligible patients were not enrolled for unclear reasons, and 577 patients could not be contacted by telephone for follow-up.

OUTCOMES MEASURED: The primary outcome measure was clinically important C-spine injury, defined as a fracture, dislocation, or ligamentous instability demonstrated by diagnostic imaging.

RESULTS: Approximately 69% of patients underwent C-spine radiography, and 31% underwent the 14-day follow-up phone interview. A total of 151 (1.7%) were determined to have a clinically important C-spine injury. No patients who did not undergo radiography were found to have important injuries 14 days later.

BACKGROUND: In the middle of the last decade several studies suggested an increased risk of thromboembolic events in women using the newer generation of oral contraceptives (OCs). These pills contain the newer progestins desogestrel, gestodene, and norgestimate. The authors of this meta-analysis attempted to address possible confounders and biases in these past studies and quantify the strength of the association.

POPULATION STUDIED: The meta-analysis included 9 case-control studies involving 3417 cases of thromboembolic disease with 9600 controls, as well as 3 cohort studies of more than 1 million women. Reported ages ranged from 15 to 49 years. All but one study (with 471 cases and 1772 controls) reported exclusion of women with a previous history of thromboembolism. Settings included hospitals, primary care offices and specialty clinics, primarily in Europe. Only studies comparing third-generation OCs to second-generation OCs were included in the final analyses.

STUDY DESIGN AND VALIDITY: The selected cohort or case-control articles were required to define cases as women with venous thrombosis or thromboembolism, and they had to contain sufficient information to determine relative risk and confidence intervals. The data were all obtained before November 1995. The study addressed possible heterogeneity among studies by stratified analysis of the results.

OUTCOMES MEASURED: The main outcome was the onset of venous embolism, comparing third-generation OC users to second-generation OC users. Because no randomized trial data were available, the investigators used odds ratios as an approximation of relative risk.

RESULTS: The study arrived at an overall adjusted odds ratio of 1.7 (95% confidence interval [CI], 1.4-2.0), a 70% higher association with thromboembolism for third-generation OCs compared with second-generation OCs. The highest odds ratio, 3.1 (95% CI, 2.0-4.6), was among first-time users. For short-term users (less than 1 year) the odds ratio was 2.5 (95% CI, 1.6-4.1), compared with 2.0 (95% CI, 1.4-2.7) for use longer than 1 year. Studies funded by the pharmaceutical industry had an odds ratio of 1.3 (95% CI, 1.0-1.7), while independent studies had an odds ratio of 2.3 (95% CI, 1.7-3.2). Age and confirmation of thromboembolism by vascular studies did not affect the odds ratios. These numbers translate to 1.5 additional incidents of thromboembolic disease per 10,000 woman years, approximately 4 additional deaths per 1,000,000 woman years. In other words, 25,000 women have to be treated over 10 years with third-generation OCs instead of second-generation OCs to expect one additional death.

BACKGROUND: In the middle of the last decade several studies suggested an increased risk of thromboembolic events in women using the newer generation of oral contraceptives (OCs). These pills contain the newer progestins desogestrel, gestodene, and norgestimate. The authors of this meta-analysis attempted to address possible confounders and biases in these past studies and quantify the strength of the association.

POPULATION STUDIED: The meta-analysis included 9 case-control studies involving 3417 cases of thromboembolic disease with 9600 controls, as well as 3 cohort studies of more than 1 million women. Reported ages ranged from 15 to 49 years. All but one study (with 471 cases and 1772 controls) reported exclusion of women with a previous history of thromboembolism. Settings included hospitals, primary care offices and specialty clinics, primarily in Europe. Only studies comparing third-generation OCs to second-generation OCs were included in the final analyses.

STUDY DESIGN AND VALIDITY: The selected cohort or case-control articles were required to define cases as women with venous thrombosis or thromboembolism, and they had to contain sufficient information to determine relative risk and confidence intervals. The data were all obtained before November 1995. The study addressed possible heterogeneity among studies by stratified analysis of the results.

OUTCOMES MEASURED: The main outcome was the onset of venous embolism, comparing third-generation OC users to second-generation OC users. Because no randomized trial data were available, the investigators used odds ratios as an approximation of relative risk.

RESULTS: The study arrived at an overall adjusted odds ratio of 1.7 (95% confidence interval [CI], 1.4-2.0), a 70% higher association with thromboembolism for third-generation OCs compared with second-generation OCs. The highest odds ratio, 3.1 (95% CI, 2.0-4.6), was among first-time users. For short-term users (less than 1 year) the odds ratio was 2.5 (95% CI, 1.6-4.1), compared with 2.0 (95% CI, 1.4-2.7) for use longer than 1 year. Studies funded by the pharmaceutical industry had an odds ratio of 1.3 (95% CI, 1.0-1.7), while independent studies had an odds ratio of 2.3 (95% CI, 1.7-3.2). Age and confirmation of thromboembolism by vascular studies did not affect the odds ratios. These numbers translate to 1.5 additional incidents of thromboembolic disease per 10,000 woman years, approximately 4 additional deaths per 1,000,000 woman years. In other words, 25,000 women have to be treated over 10 years with third-generation OCs instead of second-generation OCs to expect one additional death.

BACKGROUND: In the middle of the last decade several studies suggested an increased risk of thromboembolic events in women using the newer generation of oral contraceptives (OCs). These pills contain the newer progestins desogestrel, gestodene, and norgestimate. The authors of this meta-analysis attempted to address possible confounders and biases in these past studies and quantify the strength of the association.

POPULATION STUDIED: The meta-analysis included 9 case-control studies involving 3417 cases of thromboembolic disease with 9600 controls, as well as 3 cohort studies of more than 1 million women. Reported ages ranged from 15 to 49 years. All but one study (with 471 cases and 1772 controls) reported exclusion of women with a previous history of thromboembolism. Settings included hospitals, primary care offices and specialty clinics, primarily in Europe. Only studies comparing third-generation OCs to second-generation OCs were included in the final analyses.

STUDY DESIGN AND VALIDITY: The selected cohort or case-control articles were required to define cases as women with venous thrombosis or thromboembolism, and they had to contain sufficient information to determine relative risk and confidence intervals. The data were all obtained before November 1995. The study addressed possible heterogeneity among studies by stratified analysis of the results.

OUTCOMES MEASURED: The main outcome was the onset of venous embolism, comparing third-generation OC users to second-generation OC users. Because no randomized trial data were available, the investigators used odds ratios as an approximation of relative risk.

RESULTS: The study arrived at an overall adjusted odds ratio of 1.7 (95% confidence interval [CI], 1.4-2.0), a 70% higher association with thromboembolism for third-generation OCs compared with second-generation OCs. The highest odds ratio, 3.1 (95% CI, 2.0-4.6), was among first-time users. For short-term users (less than 1 year) the odds ratio was 2.5 (95% CI, 1.6-4.1), compared with 2.0 (95% CI, 1.4-2.7) for use longer than 1 year. Studies funded by the pharmaceutical industry had an odds ratio of 1.3 (95% CI, 1.0-1.7), while independent studies had an odds ratio of 2.3 (95% CI, 1.7-3.2). Age and confirmation of thromboembolism by vascular studies did not affect the odds ratios. These numbers translate to 1.5 additional incidents of thromboembolic disease per 10,000 woman years, approximately 4 additional deaths per 1,000,000 woman years. In other words, 25,000 women have to be treated over 10 years with third-generation OCs instead of second-generation OCs to expect one additional death.

Evidence summary

Several studies demonstrating the accuracy of helical CT have been published recently.^1-3 The most convincing are 2 prospective studies done in emergency departments in Belgium and Australia.^1,2 Both compared helical CT with intravenous pyelography (IVP) and used the gold standard of recovery and direct visualization of a stone. The Australian study enrolled 40 consecutive patients; the Belgian study enrolled 53 of 70 consecutive patients. In these 2 studies, helical CT correctly identified every instance of urinary tract stones. In contrast, IVP failed to detect stones in a third of the patients with stones, and 44% of the negative readings were false-negatives. Both tests did well in reporting negative results for those patients without stones (specificity = 97% for both tests). In terms of likelihood ratios, helical CT and IVP had positive likelihood ratios of 29 and 19, respectively, and negative likelihood ratios of 0 and 0.36 (a lower negative likelihood ratio is better). In other words, helical CT appears to be far superior to IVP in ruling out the presence of urinary tract stones. As an additional comparison, another study found that urine dipstick testing for hematuria yielded positive likelihood ratios of 1.25 and a negative likelihood ratio of 0.55.⁴ The accuracy of ultrasonography appears to fall somewhere in between hematuria testing and IVP.⁵ The Table shows an overall comparison of these diagnostic tests.

In addition to its better accuracy, several studies discuss the better safety profile and decreased diagnostic time of helical CT than IVP.^6-8 The risk of contrast reaction during IVP is between 5% and 10%, with a mortality of approximately 1 in 40,000. Helical CT (when evaluating for stones) does not use contrast, although the radiation exposure is approximately twice that of IVP.⁶ The costs of helical CT and IVP are comparable, and helical CT becomes more cost effective when the shorter time to discharge with a definitive diagnosis is considered.^7,8 Several authors also cite instances when helical CT uncovered a nonurinary cause for patients’ symptoms that IVP would have missed.^8,9

Access to helical CT is improving throughout the United States, and individual radiologists can become quickly skilled at helical CT interpretation.¹⁰ Physicians should confirm that their local radiologists are comfortable with helical CT readings before incorporating this into their diagnostic routines.

Recommendations from others

Several urology and radiology departments have published reviews lately supporting the use of helical CT over other diagnostic testing for urinary tract stones.^9,11 No official recommendations from professional organizations were found.

Evidence summary

Several studies demonstrating the accuracy of helical CT have been published recently.^1-3 The most convincing are 2 prospective studies done in emergency departments in Belgium and Australia.^1,2 Both compared helical CT with intravenous pyelography (IVP) and used the gold standard of recovery and direct visualization of a stone. The Australian study enrolled 40 consecutive patients; the Belgian study enrolled 53 of 70 consecutive patients. In these 2 studies, helical CT correctly identified every instance of urinary tract stones. In contrast, IVP failed to detect stones in a third of the patients with stones, and 44% of the negative readings were false-negatives. Both tests did well in reporting negative results for those patients without stones (specificity = 97% for both tests). In terms of likelihood ratios, helical CT and IVP had positive likelihood ratios of 29 and 19, respectively, and negative likelihood ratios of 0 and 0.36 (a lower negative likelihood ratio is better). In other words, helical CT appears to be far superior to IVP in ruling out the presence of urinary tract stones. As an additional comparison, another study found that urine dipstick testing for hematuria yielded positive likelihood ratios of 1.25 and a negative likelihood ratio of 0.55.⁴ The accuracy of ultrasonography appears to fall somewhere in between hematuria testing and IVP.⁵ The Table shows an overall comparison of these diagnostic tests.

In addition to its better accuracy, several studies discuss the better safety profile and decreased diagnostic time of helical CT than IVP.^6-8 The risk of contrast reaction during IVP is between 5% and 10%, with a mortality of approximately 1 in 40,000. Helical CT (when evaluating for stones) does not use contrast, although the radiation exposure is approximately twice that of IVP.⁶ The costs of helical CT and IVP are comparable, and helical CT becomes more cost effective when the shorter time to discharge with a definitive diagnosis is considered.^7,8 Several authors also cite instances when helical CT uncovered a nonurinary cause for patients’ symptoms that IVP would have missed.^8,9

Access to helical CT is improving throughout the United States, and individual radiologists can become quickly skilled at helical CT interpretation.¹⁰ Physicians should confirm that their local radiologists are comfortable with helical CT readings before incorporating this into their diagnostic routines.

Recommendations from others

Several urology and radiology departments have published reviews lately supporting the use of helical CT over other diagnostic testing for urinary tract stones.^9,11 No official recommendations from professional organizations were found.

Evidence summary

Several studies demonstrating the accuracy of helical CT have been published recently.^1-3 The most convincing are 2 prospective studies done in emergency departments in Belgium and Australia.^1,2 Both compared helical CT with intravenous pyelography (IVP) and used the gold standard of recovery and direct visualization of a stone. The Australian study enrolled 40 consecutive patients; the Belgian study enrolled 53 of 70 consecutive patients. In these 2 studies, helical CT correctly identified every instance of urinary tract stones. In contrast, IVP failed to detect stones in a third of the patients with stones, and 44% of the negative readings were false-negatives. Both tests did well in reporting negative results for those patients without stones (specificity = 97% for both tests). In terms of likelihood ratios, helical CT and IVP had positive likelihood ratios of 29 and 19, respectively, and negative likelihood ratios of 0 and 0.36 (a lower negative likelihood ratio is better). In other words, helical CT appears to be far superior to IVP in ruling out the presence of urinary tract stones. As an additional comparison, another study found that urine dipstick testing for hematuria yielded positive likelihood ratios of 1.25 and a negative likelihood ratio of 0.55.⁴ The accuracy of ultrasonography appears to fall somewhere in between hematuria testing and IVP.⁵ The Table shows an overall comparison of these diagnostic tests.

In addition to its better accuracy, several studies discuss the better safety profile and decreased diagnostic time of helical CT than IVP.^6-8 The risk of contrast reaction during IVP is between 5% and 10%, with a mortality of approximately 1 in 40,000. Helical CT (when evaluating for stones) does not use contrast, although the radiation exposure is approximately twice that of IVP.⁶ The costs of helical CT and IVP are comparable, and helical CT becomes more cost effective when the shorter time to discharge with a definitive diagnosis is considered.^7,8 Several authors also cite instances when helical CT uncovered a nonurinary cause for patients’ symptoms that IVP would have missed.^8,9

Access to helical CT is improving throughout the United States, and individual radiologists can become quickly skilled at helical CT interpretation.¹⁰ Physicians should confirm that their local radiologists are comfortable with helical CT readings before incorporating this into their diagnostic routines.

Recommendations from others

Several urology and radiology departments have published reviews lately supporting the use of helical CT over other diagnostic testing for urinary tract stones.^9,11 No official recommendations from professional organizations were found.