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Is one oral estrogen formulation safer than another for menopausal women?

Although numerous investigators, including the Women’s Health Initiative (WHI) team, have compared cardiovascular risks in women using menopausal hormone therapy (HT) versus nonusers, few researchers have addressed the comparative safety of different oral estrogen formulations.

Related Article: Update on Menopause (Andrew M. Kaunitz, MD, June 2013)

In this case-control study, Smith and colleagues compared the safety of oral estradiol and CEE in menopausal members of a large US Health Maintenance Organization who were using these oral estrogens between 2003 and 2009.

Details of the study
Cases were women diagnosed with deep venous thrombosis, including pulmonary embolism; myocardial infarction; or ischemic stroke. Women in the control group had no history of cardiovascular events. The endogenous thrombin potential-based normalized activated protein C sensitivity ratio (nAPCsr), which has been shown to predict venous thromboembolism (VTE) in the setting of estrogen therapy, was measured in the control group.

Between 2003 and 2009, incident VTE, MI, and stroke were diagnosed in 68, 67, and 49 cases, respectively, and 201 controls were identified. Cases were more likely than controls to have cardiovascular risk factors.

More than 90% of participants were white, with a mean age ranging from 63.2 to 67.6 years.

Among women in the control group, those using oral estradiol had slightly more cardiovascular risk factors than those using CEE, although age, body mass index, and the recency of HT initiation were similar among women using the two oral estrogens.

Although the ORs for VTE and MI were elevated among CEE users, the risk for ischemic stroke was similar for estradiol and CEE users. Women using CEE had higher nAPCsrs (P <.001), however, suggesting a greater tendency to clot.

WHAT THIS EVIDENCE MEANS FOR PRACTICE
Although the risk of VTE appears to be higher among users of oral estrogen than among those using a transdermal formulation,1 many menopausal women prefer oral estrogen for its convenience and because patch adherence can sometimes be an issue.
Oral estradiol and oral CEE appear to be equally effective in relieving menopausal symptoms. However, there is a significant cost differential: A 1-month supply of 1-mg estradiol tablets costs $4 at some chain pharmacies, whereas 0.625-mg tablets of CEE cost $84.92 (according to goodrx.com). Therefore, for menopausal women who elect to use an oral estrogen formulation, estradiol appears to be a wise choice for both safety and  economy.
Andrew M. Kaunitz, MD

WE WANT TO HEAR FROM YOU. Tell us what you think.

References

Reference

  1. Postmenopausal estrogen therapy: route of administration and risk of venous thromboembolism. Committee Opinion #556. American College of Obstetricians and Gynecologists. Obstet Gynecol. 2013;121(4):887–890.
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Andrew M. Kaunitz, MD, Professor and Associate Chairman, Department of Obstetrics and Gynecology, University of Florida College of Medicine–Jacksonville. Dr. Kaunitz serves on the OBG Management Board of Editors.

The author reports that he receives grant or research support from Agile, Bayer, Noven, and Teva, and is a consultant to Actavis, Bayer, and Teva.

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Andrew M. Kaunitz,oral estrogen,menopausal women,conjugated equine estrogens,CEE,estradiol,myocardial infarction,MI,Women’s Health Initiative,WHI,hormone therapy,HT,deep venous thrombosis,DVT,pulmonary embolism,PE,ischemic stroke,normalized activated protein C sensitivity ratio,nAPCsr,postmenopause,Examining the Evidence
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EXPERT COMMENTARY

Andrew M. Kaunitz, MD, Professor and Associate Chairman, Department of Obstetrics and Gynecology, University of Florida College of Medicine–Jacksonville. Dr. Kaunitz serves on the OBG Management Board of Editors.

The author reports that he receives grant or research support from Agile, Bayer, Noven, and Teva, and is a consultant to Actavis, Bayer, and Teva.

Author and Disclosure Information

EXPERT COMMENTARY

Andrew M. Kaunitz, MD, Professor and Associate Chairman, Department of Obstetrics and Gynecology, University of Florida College of Medicine–Jacksonville. Dr. Kaunitz serves on the OBG Management Board of Editors.

The author reports that he receives grant or research support from Agile, Bayer, Noven, and Teva, and is a consultant to Actavis, Bayer, and Teva.

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Related Articles

Although numerous investigators, including the Women’s Health Initiative (WHI) team, have compared cardiovascular risks in women using menopausal hormone therapy (HT) versus nonusers, few researchers have addressed the comparative safety of different oral estrogen formulations.

Related Article: Update on Menopause (Andrew M. Kaunitz, MD, June 2013)

In this case-control study, Smith and colleagues compared the safety of oral estradiol and CEE in menopausal members of a large US Health Maintenance Organization who were using these oral estrogens between 2003 and 2009.

Details of the study
Cases were women diagnosed with deep venous thrombosis, including pulmonary embolism; myocardial infarction; or ischemic stroke. Women in the control group had no history of cardiovascular events. The endogenous thrombin potential-based normalized activated protein C sensitivity ratio (nAPCsr), which has been shown to predict venous thromboembolism (VTE) in the setting of estrogen therapy, was measured in the control group.

Between 2003 and 2009, incident VTE, MI, and stroke were diagnosed in 68, 67, and 49 cases, respectively, and 201 controls were identified. Cases were more likely than controls to have cardiovascular risk factors.

More than 90% of participants were white, with a mean age ranging from 63.2 to 67.6 years.

Among women in the control group, those using oral estradiol had slightly more cardiovascular risk factors than those using CEE, although age, body mass index, and the recency of HT initiation were similar among women using the two oral estrogens.

Although the ORs for VTE and MI were elevated among CEE users, the risk for ischemic stroke was similar for estradiol and CEE users. Women using CEE had higher nAPCsrs (P <.001), however, suggesting a greater tendency to clot.

WHAT THIS EVIDENCE MEANS FOR PRACTICE
Although the risk of VTE appears to be higher among users of oral estrogen than among those using a transdermal formulation,1 many menopausal women prefer oral estrogen for its convenience and because patch adherence can sometimes be an issue.
Oral estradiol and oral CEE appear to be equally effective in relieving menopausal symptoms. However, there is a significant cost differential: A 1-month supply of 1-mg estradiol tablets costs $4 at some chain pharmacies, whereas 0.625-mg tablets of CEE cost $84.92 (according to goodrx.com). Therefore, for menopausal women who elect to use an oral estrogen formulation, estradiol appears to be a wise choice for both safety and  economy.
Andrew M. Kaunitz, MD

WE WANT TO HEAR FROM YOU. Tell us what you think.

Although numerous investigators, including the Women’s Health Initiative (WHI) team, have compared cardiovascular risks in women using menopausal hormone therapy (HT) versus nonusers, few researchers have addressed the comparative safety of different oral estrogen formulations.

Related Article: Update on Menopause (Andrew M. Kaunitz, MD, June 2013)

In this case-control study, Smith and colleagues compared the safety of oral estradiol and CEE in menopausal members of a large US Health Maintenance Organization who were using these oral estrogens between 2003 and 2009.

Details of the study
Cases were women diagnosed with deep venous thrombosis, including pulmonary embolism; myocardial infarction; or ischemic stroke. Women in the control group had no history of cardiovascular events. The endogenous thrombin potential-based normalized activated protein C sensitivity ratio (nAPCsr), which has been shown to predict venous thromboembolism (VTE) in the setting of estrogen therapy, was measured in the control group.

Between 2003 and 2009, incident VTE, MI, and stroke were diagnosed in 68, 67, and 49 cases, respectively, and 201 controls were identified. Cases were more likely than controls to have cardiovascular risk factors.

More than 90% of participants were white, with a mean age ranging from 63.2 to 67.6 years.

Among women in the control group, those using oral estradiol had slightly more cardiovascular risk factors than those using CEE, although age, body mass index, and the recency of HT initiation were similar among women using the two oral estrogens.

Although the ORs for VTE and MI were elevated among CEE users, the risk for ischemic stroke was similar for estradiol and CEE users. Women using CEE had higher nAPCsrs (P <.001), however, suggesting a greater tendency to clot.

WHAT THIS EVIDENCE MEANS FOR PRACTICE
Although the risk of VTE appears to be higher among users of oral estrogen than among those using a transdermal formulation,1 many menopausal women prefer oral estrogen for its convenience and because patch adherence can sometimes be an issue.
Oral estradiol and oral CEE appear to be equally effective in relieving menopausal symptoms. However, there is a significant cost differential: A 1-month supply of 1-mg estradiol tablets costs $4 at some chain pharmacies, whereas 0.625-mg tablets of CEE cost $84.92 (according to goodrx.com). Therefore, for menopausal women who elect to use an oral estrogen formulation, estradiol appears to be a wise choice for both safety and  economy.
Andrew M. Kaunitz, MD

WE WANT TO HEAR FROM YOU. Tell us what you think.

References

Reference

  1. Postmenopausal estrogen therapy: route of administration and risk of venous thromboembolism. Committee Opinion #556. American College of Obstetricians and Gynecologists. Obstet Gynecol. 2013;121(4):887–890.
References

Reference

  1. Postmenopausal estrogen therapy: route of administration and risk of venous thromboembolism. Committee Opinion #556. American College of Obstetricians and Gynecologists. Obstet Gynecol. 2013;121(4):887–890.
Issue
OBG Management - 26(1)
Issue
OBG Management - 26(1)
Page Number
50-51
Page Number
50-51
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Display Headline
Is one oral estrogen formulation safer than another for menopausal women?
Display Headline
Is one oral estrogen formulation safer than another for menopausal women?
Legacy Keywords
Andrew M. Kaunitz,oral estrogen,menopausal women,conjugated equine estrogens,CEE,estradiol,myocardial infarction,MI,Women’s Health Initiative,WHI,hormone therapy,HT,deep venous thrombosis,DVT,pulmonary embolism,PE,ischemic stroke,normalized activated protein C sensitivity ratio,nAPCsr,postmenopause,Examining the Evidence
Legacy Keywords
Andrew M. Kaunitz,oral estrogen,menopausal women,conjugated equine estrogens,CEE,estradiol,myocardial infarction,MI,Women’s Health Initiative,WHI,hormone therapy,HT,deep venous thrombosis,DVT,pulmonary embolism,PE,ischemic stroke,normalized activated protein C sensitivity ratio,nAPCsr,postmenopause,Examining the Evidence
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