Angeliq (drospirenone and estradiol) is a female hormone that is commonly used to reduce the symptoms associated with menopause such as hot flashes and other vasomotor symptoms.
Angeliq (Drospirenone and estradiol) Uses:
-
Vasomotor symptoms associated with menopause:
- Treatment of moderate to severe vasomotor symptoms associated with menopause in women with a uterus.
-
Vulvar and vaginal atrophy associated with menopause:
- Treatment of moderate to severe vulvar and vaginal because of menopause in women with a uterus.
- Limitations of use:
- When used as monotherapy for the treatment of vulvar and vaginal atrophy, topical vaginal products should be considered.
Note:
- The International Society for the Study of Women’s Sexual Health and The North American Menopause Society has endorsed the term genitourinary syndrome of menopause (GSM) as new terminology for vulvovaginal atrophy.
- The term GSM includes all genital and urinary signs and symptoms associated with a loss of estrogen because of menopause.
Adult dose:
Angeliq (drospirenone and estradiol) General dosing guidelines:
- When treating symptoms of menopause, hormone therapy should be evaluated routinely for appropriate dose, duration, and route of administration for each individual patient according to treatment goals, risk factors, and overall health.
Angeliq (drospirenone and estradiol) Dose in the treatment of Vasomotor symptoms associated with menopause:
- Oral: Drospirenone 0.25 mg/estradiol 0.5 mg or drospirenone 0.5 mg/estradiol 1 mg per tablet: One tablet daily.
Angeliq (drospirenone and estradiol) Dose in the treatment of Vulvar and vaginal atrophy associated with menopause:
- Oral: Drospirenone 0.5 mg/estradiol 1 mg per tablet: One tablet daily.
Use in Children:
Not indicated.
Pregnancy Risk Category: X
- Contraindicated for pregnant women
Breastfeeding: Drospirenone or estradiol
- Breast milk contains drospirone.
- The infant received a maximum dose of 3 mg/day of drospirenone after being administered an oral contraceptive drug containing drospirenone.
- Breast milk quality and quantity may be affected by estrogens.
Dose in Kidney disease:
Use is contraindicated.
Dose in Liver disease:
Use is contraindicated.
Common Side Effects of Angeliq (Drospirenone and estradiol):
-
Genitourinary:
- Mastalgia
- Genital bleeding
Less Common Side Effects of Angeliq (Drospirenone and estradiol):
-
Central nervous system:
- Emotional lability
- Migraine
-
Gastrointestinal:
- Abdominal pain
- Gastrointestinal pain
-
Genitourinary:
- Cervical polyp
Contraindications to Angeliq (Drospirenone and estradiol):
- Angioedema, angioedema or anaphylactic reaction to drospirenone or estradiol or any component of formulation.
- Undiagnosed abnormal Genital Bleeding;
- DVT or PE (current and/or historical of);
- Active or past history of arterial embombolic disease (eg stroke, MI)
- Breast carcinoma (known, suspected or history of);
- An estrogen-dependent tumor (known, suspected)
- Hepatic impairment or disease
- Renal impairment
- Insufficiency of adrenal;
- Protein C, protein S, and other known thrombophilic conditions;
- Confirmed or suspected pregnancy
Canadian labeling: Additional contraindications not in US labeling
- Progestin-dependent malignant Neoplasia (current and/or history of);
- Malignant or benign liver tumors (currently or in the past);
- Endometrial hyperplasia
- severe hypertriglyceridemia;
- Classic migraine
- Ophthalmic vascular disease can cause vision loss, partial or total.
- Breastfeeding
Warnings and precautions
-
[US Boxed Warning] Breast Cancer
- Data from the Women's Health Initiative (WHI), shows that postmenopausal women who use conjugated estrogens (CE) and medroxyprogesterone (MPA) have a higher risk of developing invasive breast cancer.
- Studies have shown that stopping therapy reduces the risk.
- The WHI study didn't report an increase in breast cancer risk for women who had a hysterectomy with CE.
- Postmenopausal women receiving hormone therapy could be at greater risk for breast cancer due to their estrogen or progestin doses, timing of therapy initiation, length of therapy, route of administration and patient characteristics.
- Increased breast density may be caused by hormone therapy.
- An increase in abnormal mammogram findings that require further evaluation has been reported using estrogen alone or in combination.
- Patients with breast cancer or bone metastases may experience severe hypercalcemia from estrogen use. If this happens, discontinue estrogen.
-
Dementia: [US Boxed Warning]
- To prevent dementia, it is not a good idea to use estrogens without or with progestin.
- The Women's Health Initiative Memory Study, (WHIMS), found that women aged >=65 years were more likely to develop dementia if they took CE either alone or in combination.
- The WHI memory studies were performed on women aged >=65 years. It is not known if the findings can be applied to younger postmenopausal females.
- Hormone therapy is not recommended for any age in order to treat or prevent cognitive decline or dementia.
-
Endometrial Cancer: [US Boxed Warn]
- Endometrial cancer is more likely to occur in women who use unopposed estrogen.
- A progestin may be added to estrogen therapy to reduce the chance of endometrial hyperplasia. This is a precursor for endometrial carcinoma.
- To rule out malignancy in women who have undiagnosed abnormal vaginal blood flow, it is important to perform appropriate diagnostic tests, including endometrial sampling, if necessary.
- Estrogens may exacerbate endometriosis.
- Post-hysterectomy with estrogen therapy unopposed has led to malignant transformation of the remaining endometrial implants.
- Women with endometrium after hysterectomy should consider adding a progestin.
- There is no evidence to suggest that natural estrogens have a different risk profile than synthetic estrogens of equivalent estrogen doses.
- Endometrial cancer risk appears to be dependent on the duration and dose of treatment. It is highest for patients who have been using therapy for more than 5 years. This may continue even after discontinuation.
- A progestin should not be used if low doses are being administered locally to treat vaginal atrophy. However, there are insufficient long-term data (>1 years) to support this recommendation.
-
Endometriosis:
- Estrogens may exacerbate endometriosis.
- Post-hysterectomy with estrogen therapy unopposed has led to malignant transformation of the remaining endometrial implants.
- Women with endometriosis after hysterectomy should consider adding a progestin.
-
Hyperkalemia:
- Drospirenone may cause hyperkalemia by its anti-mineralocorticoid activity.
- Patients with hyperkalemia-predisposing conditions (eg, renal dysfunction, hepatic dysfunction or adrenal insufficiency) should not use this medication.
-
Hyponatremia:
- Hyponatremia may be increased by Drospirenone in high-risk patients.
-
The Lipid Effects
- Estrogen compounds have lipid effects, such as higher HDL-cholesterol or decreased LDL cholesterol.
- Triglycerides may also be increased in women with preexisting hypertriglyceridemia; cease if pancreatitis occurs.
- Patients with familial lipoprotein metabolism defects should be cautious.
-
Ovarian cancer:
- The information available regarding the risk of ovarian carcinoma and the use of estrogen/progestin therapy or menopausal estrogen is not consistent.
- An association may exist, but the risk of developing a serious condition is unlikely. The duration of therapy can also influence the likelihood of developing a severe reaction.
-
Retinal vascular embolism:
- Estrogens can cause retinal vein thrombosis. Discontinue use if you experience migraines, vision loss, proptosis or diplopia. If retinal vascular or papilledema on examination, discontinue use permanently.
-
Asthma
- Patients with asthma should exercise caution as it can worsen the condition.
-
Carbohydrate intolerance:
- Patients with diabetes may experience impaired glucose tolerance.
- Take into account the age, cardiovascular and metabolic risk factors of patients with diabetes.
-
Cardiovascular disease: [US-Boxed Warning]
- To prevent heart disease, estrogens should not be combined with or without progestin.
- Data from the Women's Health Initiative's (WHI) studies has shown that CE has an increased risk for stroke and deep vein thrombosis. There has also been an increase in DVT, stroke, and pulmonary emboli (PE) in postmenopausal females between 50 and 79 years old.
- Additional risk factors include diabetes mellitus, hypercholesterolemia, hypertension, SLE, obesity, tobacco use, and/or history of venous thromboembolism (VTE).
- It is important to manage risk factors properly. If adverse cardiovascular events are suspected or occur, it is best to stop immediately.
- Transdermal administration is preferred to treat vasomotor symptoms associated with menopause in patients at high risk for developing thrombotic events.
- Women with an active DVT, PE, or arterial thromboembolic diseases (stroke and MI) are not recommended.
-
Chorea minor:
- Chorea minor should be used with caution as it can exacerbate the condition.
-
Fluid retention can lead to more severe diseases
- Patients with fluid retention-related diseases, such as cardiac or renal dysfunction, should be cautious.
-
Epilepsy:
- Epilepsy can be exacerbated by caution.
-
Gallbladder disease
- Postmenopausal estrogen use may increase the risk of gallbladder diseases that require surgery.
-
Hepatic dysfunction
- Patients with hepatic dysfunction are less likely to be able to metabolize estrogens.
- Be cautious if you have a history of cholestatic jaundice due to previous estrogen use or pregnancy.
- If jaundice occurs or if there are acute or chronic hepatic disorders, discontinue use.
- Hepatic impairment and disease are reasons for the contraindication of using this medication.
-
Hepatic hemomangiomas
- Patients with hepatic hemomangiomas should be cautious; it may worsen the condition.
-
Hereditary angioedema:
- Women with hereditary angioedema may experience angioedema symptoms from exogenous estrogens.
-
Hypoparathyroidism:
- Hypoparathyroidism patients should be cautious; estrogen-induced hypocalcemia can occur.
-
Migraine
- Patients suffering from migraines should be cautious. It may worsen the condition.
-
Otosclerosis
- Be cautious with otosclerosis. It can worsen the condition.
-
Porphyria
- Patients with porphyria should be cautious; it may worsen the condition.
-
SLE:
- Patients with SLE should be cautious; it may worsen the condition.
Drospirenone and estradiol: Drug Interaction
Note: Drug Interaction Categories:
- Risk Factor C: Monitor When Using Combination
- Risk Factor D: Consider Treatment Modification
- Risk Factor X: Avoid Concomitant Use
Risk Factor C (Monitor therapy). |
|
Ajmaline | Ajmaline's toxic/adverse effects may be exacerbated by Estrogen Derivatives. Particularly, there may be an increase in the risk of cholestasis. |
Aliskiren | Drospirenone could increase the hyperkalemic effects of Aliskiren. |
Angiotensin II Receptor Blockers | Might increase the hyperkalemic effects of Drospirenone. |
Angiotensin-Converting Enzyme Inhibitors | Might increase the hyperkalemic effects of Drospirenone. |
Anthrax Immune Globulin (Human) | Anthrax Immune Globulin (Human) may have a thrombogenic effect due to Estrogen Derivatives. |
Antidiabetic Agents | Hyperglycemia-Associated Agents may diminish the therapeutic effect of Antidiabetic Agents. |
Ascorbic Acid | May increase serum Estrogen Derivatives concentrations. |
Broccoli | High risk of Inducers causing a decrease in serum CYP1A2 Substrates concentrations |
C1 inhibitors | The thrombogenic effects of C1 inhibitors could be enhanced by Estrogen Derivatives. |
C1 inhibitors | The thrombogenic effects of C1 inhibitors could be enhanced by progestins. |
Cannabis | High risk of Inducers causing a decrease in serum CYP1A2 Substrates concentrations |
Chenodiol | The therapeutic effects of Chenodiol may be diminished by the use of estrogen derivatives. When using chenodiol in combination with estrogen derivatives, be sure to monitor your clinical response. |
CloZAPine | CloZAPine serum concentrations may be increased by CYP1A2 inhibitors (Weak). Management: The drug interactions monographs for drugs listed as an exception to this monograph will discuss the management of these drugs. |
Corticosteroids (Systemic) | Estrogen Derivatives can increase serum levels of Corticosteroids Systemic. |
Moderate CYP1A2 Inducers | High risk of Inducers causing a decrease in serum CYP1A2 Substrates concentrations |
Moderate CYP3A4 Inducers | Could lower serum concentrations of CYP3A4 substrates (High Risk with Inducers). |
Moderate CYP3A4 inhibitors | May increase serum Estrogen Derivatives concentrations. |
Cyproterone | High risk of Inducers causing a decrease in serum CYP1A2 Substrates concentrations |
Dantrolene | Dantrolene's hepatotoxic effects may be increased by Estrogen Derivatives. |
Deferasirox | Could lower serum concentrations of CYP3A4 substrates (High Risk with Inducers). |
Erdafitinib | Could lower serum concentrations of CYP3A4 substrates (High Risk with Inducers). |
Erdafitinib | Increased serum concentrations of P-glycoprotein/ABCB1 Substrates may be possible. |
Flibanserin | Flibanserin can be increased by contraceptives and progestins. |
Herbs (Estrogenic Properties) | May increase the toxic/adverse effects of Estrogen Derivatives. |
Herbs with Progestogenic Properties (eg Bloodroot, Yucca). | Progestins may have an adverse/toxic effect that can be increased. |
Immune Globulin | The thrombogenic effects of Immune Globulin may be enhanced by Estrogen Derivatives. |
LamoTRIgine | May lower the serum level of Progestins (Contraceptive). |
LamoTRIgine | The serum level of LamoTRIgine may be decreased by Estrogen Derivatives |
Lenalidomide | The thrombogenic effects of Lenalidomide may be enhanced by Estrogen Derivatives. |
Metreleptin | May lower the serum level of Progestins (Contraceptive). Metreleptin can increase the serum Progestins concentration (Contraceptive). |
Mivacurium | The serum concentrations of Mivacurium may be increased by Estrogen Derivatives. |
Nonsteroidal Anti-Inflammatory Drugs | Might increase the hyperkalemic effects of Drospirenone. |
P-glycoprotein/ABCB1 Inhibitors | Increases serum concentrations of Pglycoprotein/ABCB1 substrates. P-glycoprotein inhibitors can also increase the distribution of pglycoprotein substrates to certain cells/tissues/organs in which p-glycoprotein exists in high amounts (e.g. brain, T-lymphocytes and testes). . |
Potassium-Sparing Diuretics | Drospirenone could increase the hyperkalemic effects of PotassiumSparing Diuretics. |
Ranolazine | Increased serum concentrations of P-glycoprotein/ABCB1 Substrates may be possible. |
ROPINIRole | The serum concentrations of ROPINIRole may be increased by Estrogen Derivatives. |
Sarilumab | Could lower serum concentrations of CYP3A4 substrates (High Risk with Inducers). |
Selegiline | The serum concentrations of Selegiline may be increased by contraceptives (progestins). |
Siltuximab | Could lower serum concentrations of CYP3A4 substrates (High Risk with Inducers). |
Succinylcholine | The serum concentrations of succinylcholine may be increased by Estrogen Derivatives. |
Teriflunomide | High risk of Inducers causing a decrease in serum CYP1A2 Substrates concentrations |
Thalidomide | Thalidomide's thrombogenic effects may be enhanced by contraceptives (progestins). |
Thalidomide | Thalidomide may have a thrombogenic effect that Estrogen Derivatives can enhance. |
Theophylline Derivatives | The serum concentrations of Theophylline Derivatives could be increased by Estrogen Derivatives. Dyphylline is an exception. |
Thyroid Products | Thyroid products may be less effective if they contain Estrogen Derivatives. |
Tocilizumab | Could lower serum concentrations of CYP3A4 substrates (High Risk with Inducers). |
Ursodiol | The therapeutic effects of Ursodiol may be diminished by Estrogen Derivatives. |
Risk Factor D (Regard therapy modification) |
|
Acitretin | Progestins may have a lower therapeutic effect (Contraceptive). It is possible to have contraceptive failure. Management: Progestin-only products may not prevent pregnancy. Alternative contraception methods, including nonhormonal ones, must be used during acitretin treatment. |
Anticoagulants | Estrogen Derivatives can decrease the anticoagulant effects of Anticoagulants. Progestin-estrogen combination and estrogens may have prothrombotic properties that counteract anticoagulant effects. Management: Consider the potential benefits of estrogens in relation to the increased risk of thromboembolism and procoagulant effects. Some circumstances may make estrogens contraindicated. For more information, refer to the guidelines. |
Anticoagulants | Anticoagulants may be less effective when used in combination with progestins. Progestin-estrogen combination and some progestins may have prothrombotic side effects that could counteract anticoagulant properties. Management: Consider the pros and cons of progestins in relation to the possible increased risk of thromboembolism or procoagulant effects. Some circumstances may make progestins contraindicated. For more information, refer to the guidelines. |
Aprepitant | May cause a decrease in serum progestin levels (Contraceptive). Management: Alternative or additional methods of contraception should be used both during treatment with aprepitant or fosaprepitant and for at least one month following the last aprepitant/fosaprepitant dose. |
Artemether | Could lower serum levels of Progestins (Contraceptive). Management: All women with childbearing potential that are currently using artemether should consider a non-hormonal method of contraception. |
Atazanavir | May increase serum levels of Progestins (Contraceptive). Atazanavir can reduce the effectiveness of oral contraceptive medications and ethinyl ester concentrations. Management: You may consider an alternative or additional method to contraception, especially if you are using combined estrogen/progestin products. You may use depot medroxyprogesteronecetate without the need for additional contraception. |
Barbiturates | Progestins may have a lower therapeutic effect (Contraceptive). It is possible to have contraceptive failure. Management: It is recommended to use nonhormonal contraceptives. |
Bexarotene (Systemic) | May lower the serum concentrations of Progestins (Contraceptive). Management: Bexarotene-treated women with childbearing potential should use at least two forms of reliable contraception, including one that is nonhormonal. |
Bile Acid Sequestrants | May cause a decrease in serum progestin levels (contraceptive). Administration: Oral progestin-containing contraceptives should be administered at least one to four hours before or after the administration of a sequestrant bile acid. |
Bosentan | Can decrease serum progestin levels (Contraceptive). Management: All women with childbearing potential using bosentan should use an alternative, or non-hormonal, method of contraception. Do not rely solely on hormonal contraceptives. |
Brigatinib | Can decrease serum progestin levels (Contraceptive). Management: Females with childbearing potential should consider using a non-hormonal contraceptive for at least four months following the last brigatinib treatment. |
CarBAMazepine | Progestins may have a lower therapeutic effect (Contraceptive). It is possible to have contraceptive failure. Management: It is recommended to use nonhormonal contraceptives. |
Carfilzomib | Progestins may increase the risk of thrombogenic effects (Contraceptive). Treatment: Patients who are undergoing carfilzomib therapy should consider other, non-hormonal contraceptive methods. |
Cladribine | This may reduce the therapeutic effects of Hormonal contraceptives. Management: Women who use hormonal contraceptives that systemically act should be aware of the need to add a barrier method for at least four weeks following each dose. |
CloBAZam | May lower the serum level of Progestins (Contraceptive). |
Cobicistat | Increased serum levels of Progestins (Contraceptive) may be possible. Treatment: Patients who are cobicistat-containing should consider an alternative contraceptive. Drospirenone is contraindicated when taken with cobicistat and atazanavir. |
Cosyntropin | The diagnostic value of Cosyntropin may be diminished by Estrogen Derivatives. Management: Stop using estrogen-containing drugs for 4 to 6 weeks before you undergo cosyntropin testing (ACTH). |
Strong CYP3A4 Inducers | May increase metabolism of CYP3A4 substrates (High Risk with Inducers). Management: You may consider a different drug to replace one of the interacting drugs. Some combinations might be contraindicated. Consult appropriate manufacturer labeling. |
Strong CYP3A4 inhibitors | Increased serum levels of Drospirenone. Concurrent use of Drospirenone is not recommended. This is because the strong CYP3A4 inhibitors atazanavir (and cobicistat) are being administered simultaneously. When drospirenone coadministered alongside other strong CYP3A4 inhibitors, it is important to exercise caution. |
Dabrafenib | High risk of Inducers causing a decrease in serum CYP3A4 substrates. Management: If possible, seek alternatives to the CYP3A4 substrate. Concomitant therapy should be avoided if possible. Monitor the clinical effects of the substrate carefully (especially therapeutic effects). |
Dabrafenib | May lower the serum concentrations of Progestins (Contraceptive). Management: Females with reproductive potential should consider an alternative, non-hormonal method of contraception. This can be used during or after 2 weeks (dabrafenib only) or 4 months (dabrafenib and trametinib combined). |
Darunavir | The serum concentration of Progestins may be decreased (Contraceptive). Management: You may consider using another method of contraception. You may use injectable depot medroxyprogesteronecetate acetate without the need for additional contraception. |
Efavirenz | Could cause a decrease in serum levels of Progestins (Contraceptive). Management: Consider using an alternative or more effective method of contraception to reduce the effectiveness of your contraceptive. This interaction does not appear to be possible with injectable depot medroxyprogesterone. |
Enzalutamide | High risk of Inducers causing a decrease in serum concentrations of CYP3A4 substrates. Management: Avoid concurrent use of enzalutamide and CYP3A4 substrates with a narrow therapeutic index. You should exercise caution when using enzalutamide or any other CYP3A4 sub-substance. |
Eslicarbazepine | Could lower the serum level of Progestins (Contraceptive). Management: Women with child-bearing potential should consider other, non-hormonal methods of birth control. |
Exenatide | Progestins may be lower in the blood (oral contraceptive). Administration: Take oral contraceptives at the least one hour before you take exenatide. |
Felbamate | May cause a decrease in serum Progestin levels (Contraceptive). Management: It is possible to have contraceptive failure. It is possible to use a nonhormonal contraceptive method. |
Fosamprenavir | Fosamprenavir may be decreased by contraceptives and progestins. Fosamprenavir can decrease serum concentrations of Progestins. Management: You may consider using another method of contraception. You may use injectable depot medroxyprogesteronecetate acetate without the need for additional contraception. |
Fosaprepitant | May cause a decrease in serum Progestins (Contraceptive). This effect is most likely due to the active metabolite, aprepitant. Management: Alternative or additional methods of contraception should be used both during treatment with aprepitant or fosaprepitant and for at least one month following the last aprepitant/fosaprepitant dose. |
Fosphenytoin | Progestins may have a lower therapeutic effect (Contraceptive). It is possible to have contraceptive failure. Management: Contraceptive Failure is possible. It is recommended to use a nonhormonal contraceptive. |
Hyaluronidase | Hyaluronidase's therapeutic effects may be diminished by Estrogen Derivatives. Treatment: Hyaluronidase may not be effective in patients who are taking estrogens, especially at higher doses. Higher doses of hyaluronidase might be necessary. |
Ivosidenib | Progestins may be reduced in the serum (Contraceptive). Treatment: Patients receiving ivosidenib should consider other methods of contraception, i.e. non-hormonal. |
Lesinurad | Could lower the serum level of Progestins (Contraceptive). Patients who are being treated with Lesinurad should consider a nonhormonal contraceptive if they desire to use effective contraception. |
Lixisenatide | Could cause a decrease in serum Progestin levels (Contraceptive). Administration: Oral contraceptives should be administered at least one hour before, or 11 hours after, administration of lixisenatide. |
Lopinavir | May lower the serum level of Progestins (Contraceptive). Lopinavir can increase the serum level of Progestins (Contraceptive). Management: You may consider using another method of contraception. You can use etonogestrel and depot medroxyprogesterone Acetate injections without the need for additional contraception. |
Lorlatinib | High risk of Inducers causing a decrease in serum concentrations of CYP3A4 substrates. Management: Do not use lorlatinib concurrently with any CYP3A4 Substrates. Even a slight decrease in serum concentrations could cause therapeutic failure or serious clinical consequences. |
Lumacaftor | The serum concentration of Progestins may be decreased (Contraceptive). Management: Do not rely on hormone-based contraceptives with concurrent use of lumacaftor/ivacaftor; an alternative, non-hormonal, method of contraception should be used if this combination is required. |
MiFEPRIStone | May decrease the therapeutic effects of Progestins. MiFEPRIStone can increase serum Progestins (Contraceptive). Management: Women with childbearing potential need to use a nonhormonal, effective contraceptive during and after mifepristone treatment. |
Mitotane | High risk of Inducers causing a decrease in serum concentrations of CYP3A4 substrates. Treatment: Patients receiving mitotane may require significant adjustments in the dosage of CYP3A4 Substrates. |
Mycophenolate | Progestin levels may be lower (Contraceptive). Management: It is recommended to consider a nonhormonal method of contraception. |
Nelfinavir | Could cause a decrease in serum levels of Progestins (Contraceptive). Management: Consider using an alternative or more effective method of contraception to reduce the effectiveness of your contraceptive. This interaction does not appear to be possible with injectable depot medroxyprogesterone. |
Nevirapine | Progestins may be reduced in the serum (Contraceptive). Patients receiving nevirapine should be instructed to use an alternate or non-hormonal contraceptive. Nevirapine product labeling however suggests that depo-medroxyprogesterone acetate may be used as a sole method of contraception. |
OXcarbazepine | May cause a decrease in serum Progestin levels (Contraceptive). Management: It is possible to have contraceptive failure. It is possible to use a nonhormonal contraceptive method as an alternative. |
Perampanel | May cause a decrease in serum levels of Progestins (Contraceptive). Treatment: Patients should consider a nonhormonal contraceptive for the duration of perampanel use and up to one month after stopping it. |
Phenytoin | Progestins may have a lower therapeutic effect (Contraceptive). It is possible to have contraceptive failure. Management: Contraceptive Failure is possible. It is recommended to use a nonhormonal contraceptive. |
Pitolisant | Progestins may have a lower therapeutic effect (Contraceptive). Management: Avoid using hormonal contraceptives that combine pitolisant and hormonal contraceptives. Instead, you should use an alternative method of contraception. |
Pitolisant | High risk of Inducers causing a decrease in serum concentrations of CYP3A4 substrates Management: Avoid combining pitolisant and a CYP3A4 substrat with a low therapeutic index. Pitolisant should not be combined with other CYP3A4 sub-substances. |
Pomalidomide | Estrogen Derivatives may increase the risk of thrombogenesis. Management: The Canadian pomalidomide labeling advises caution when using hormone replacement therapy. It also states that hormonal contraceptives should not be used. These recommendations are not included in the US pomalidomide labeling. |
Pomalidomide | Pomalidomide's thrombogenic effects may be enhanced by progestins. Management: The Canadian Pomalidomide Labeling advises caution when using hormone replacement therapy. It also states that hormonal contraceptives should not be used. These recommendations are not included in the US pomalidomide labeling. |
Primidone | Progestins may have a lower therapeutic effect (Contraceptive). It is possible to have contraceptive failure. Management: It is recommended to use nonhormonal contraceptives. |
Retinoic Acid Derivatives | Progestins may have a lower therapeutic effect (Contraceptive). The serum concentration of Progestins can be decreased by Retinoic Acid derivatives (Contraceptive). Patients who are taking retinoic acid derivatives should use two forms of effective contraception. Microdosed progesterone-only formulations might not be as effective, in particular. Exceptions: Adapalene; Bexarotene (Topical); Tretinoin (Topical). |
Rifamycin Derivatives | May cause a decrease in serum Progestin levels (Contraceptive). It is possible to have contraceptive failure. Management: Contraceptive Failure is possible. It is recommended to use a nonhormonal contraceptive. |
Saquinavir | Could cause a decrease in serum levels of Progestins (Contraceptive). Management: Consider using an alternative or more effective method of contraception to reduce the effectiveness of your contraceptive. This interaction does not appear to be possible with injectable depot medroxyprogesterone. |
Somatropin | Somatropin's therapeutic effects may be diminished by Estrogen Derivatives. This is a concern for women who use oral hormone replacement therapy after menopause. Management: Watch out for a decrease in growth hormone efficacy. To reach the treatment goal, a higher dose of somatropin may be necessary. This interaction appears to not apply to non-oral estrogens (e.g. transdermal or vaginal rings). |
St John's Wort | Progestins may have a lower therapeutic effect (Contraceptive). Contraceptive failure can occur. Management: You might consider using another product than St John's Wort. It is possible to have a contraceptive fail. It is recommended to use a nonhormonal contraceptive. |
St John's Wort | High risk of Inducers causing a decrease in serum CYP3A4 Substrates. Management: You may consider a different drug to replace one of the interacting drugs. Some combinations might be contraindicated. Consult appropriate manufacturer labeling. |
Sugammadex | The serum concentration of Progestins may be decreased (Contraceptive). Treatment: Patients who have received any hormonal contraceptive (oral and non-oral), should continue to use a nonhormonal contraceptive method for at least 7 days after sugammadex treatment. |
Tipranavir | Tipranavir's dermatologic side effects may be exacerbated by Estrogen Derivatives. The combination of tipranavir/ritonavir and ethinyl estradiol/norethindrone was associated with a high incidence of skin rash. Tipranavir can lower the serum Estrogen Derivatives concentration. Management: Women who use hormonal contraceptives need to consider non-hormonal contraceptives. |
Tipranavir | Increased serum levels of Progestins may be a contraceptive. Management: Consider using an alternative or more effective method of contraception to reduce the effectiveness of your contraceptive. This interaction does not appear to be possible with injectable depot medroxyprogesterone. |
TiZANidine | CYP1A2 Inhibitors, Weak, may increase serum TiZANidine concentrations. These combinations should be avoided whenever possible. Begin tizanidine in adults at 2 mg. Then, increase the dose according to patient response. Be aware of any adverse reactions and increased effects of tizanidine. |
Topiramate | May cause a decrease in serum Progestin levels (Contraceptive). Patients should be aware that this combination can reduce contraceptive effectiveness. You may want to consider adding a non-hormonal contraceptive method. |
Vitamin K antagonists (eg warfarin) | Vitamin K Antagonists may be affected by contraceptives, such as estrogens. Some products have shown enhanced anticoagulant properties. Management: Concomitant hormonal contraceptives or coumarin derivatives should not be used if possible to avoid thromboembolic complications. You might consider using a nonhormonal contraceptive. |
Risk Factor X (Avoid Combination) |
|
Anastrozole | Anastrozole's therapeutic effects may be diminished by Estrogen Derivatives. |
Dehydroepiandrosterone | May increase the toxic/adverse effects of Estrogen Derivatives. |
Encorafenib | May lower the serum level of Progestins (Contraceptive). |
Exemestane | Exemestane's therapeutic effects may be diminished by Estrogen Derivatives. |
Griseofulvin | Progestins may have a lower therapeutic effect (Contraceptive). It is possible to have contraceptive failure. |
Hemin | Hemin's therapeutic effects may be diminished by Estrogen Derivatives |
Indium 111 Capromab Pendetide | Indium 111 Capromab Pendetide may be less effective in diagnosing a condition known as Estrogen Derivatives. |
Ixazomib | May lower the serum concentrations of Progestins (Contraceptive). Particularly, ixazomib combined with dexamethasone can decrease serum progestin levels. Treatment: Women with childbearing potential must use a nonhormonal contraceptive for at least 90 days after ixazomib treatment. |
Ospemifene | Ospemifene's toxic/adverse effects may be increased by Estrogen Derivatives. Ospemifene's therapeutic effects may be diminished by Estrogen Derivatives. |
Tranexamic acid | Tranexamic Acid may increase the risk of thrombosis by using contraceptives (progestins). |
Ulipristal | Progestins can decrease the therapeutic effects of Ulipristal. Progestins may be less effective when Ulipristal is used. Management: Ulipristal is indicated for the treatment of uterine fibroids in Canada. Progestins should be stopped within 12 days. As an emergency contraceptive, (U.S. indication), progestins should be stopped within 5 days. |
Monitoring parameters:
- Before therapy, baseline risk for breast cancer and CVD.
- During therapy, age-appropriate breast, and pelvic exams;
- blood pressure;
- unscheduled bleeding lasting >6 months for endometrial pathology (sooner in patients who are obese, diabetic, or have a history of endometrial cancer);
- serum triglycerides (2 weeks after starting therapy in patients with baseline level >200 mg/dL);
- TSH (6 to 12 weeks after starting oral therapy in patients taking thyroid replacement).
- Efficacy beginning 1 to 3 months after starting therapy, then every 6 to 12 months as appropriate.
- The duration of treatment should be evaluated at least yearly.
- Serum potassium during the first month of therapy in patients at risk for hyperkalemia and who are on chronic strong CYP3A4 inhibitors
Note: Monitoring of FSH and serum estradiol is not useful when managing vasomotor symptoms or GSM
How to administer Angeliq (Drospirenone and estradiol)?
- Tablets should be swallowed whole with some liquid with or without meals and taken at the same time every day.
- Bleeding may occur if several doses are missed. Women who are not taking estrogen or who are changing from a continuous combination product may begin therapy at any time.
- Women who are switching from sequential or cyclic hormone therapy should complete the current cycle before switching to this product.
- A forgotten dose should be taken as soon as possible. If more than 24 hours have elapsed, the missed tablet should not be taken.
Mechanism of action of Angeliq (Drospirenone and estradiol):
Drospirenone is a synthetic progestin and spironolactone analog with anti-mineralocorticoid and antiandrogenic activity. It counteracts estrogen-induced endometrial thinning. Estrogens are responsible to the development and maintenance the female reproductive system as well as secondary sexual characteristics.
Estradiol is the principal intracellular human estrogen and is stronger than estrone and estriol at the receptor level; it is the primary estrogen secreted before menopause. Estrone and estrone-sulfate become more abundant after menopause.
Through a negative feedback mechanism, estrogens regulate the pituitary secretion gonadotropins,luteinizing hormone and follicle stimulating hormone. Postmenopausal women with high levels of estrogen replace these hormones.
Protein binding:
- Drospirenone: 97%;
- does not bind to sex hormone-binding globulin or corticosteroid-binding globulin
- Estradiol: 37% bound to sex hormone-binding globulin;
- 61% bound to albumin
Metabolism:
- Hepatic
- Drospirenone forms two metabolites (inactive)
- Estradiol: Converted to estrone and estriol; also undergoes enterohepatic recirculation; estrone sulfite is the main metabolite in postmenopausal women
Bioavailability:
- Drospirenone: 76% to 85%
Half-life elimination:
- Drospirenone: ~36-42 hours
Time to peak, plasma:
- Drospirenone: 1 hour;
- Estradiol: ~2 hours (range: 0.3-10 hours)
Excretion:
- Drospirenone: Urine and feces;
- Estradiol: Urine
International Brand Names of Drospirenone and estradiol:
- Angeliq
- Angelica
- Angemin
- AST
- Astarte
Drospirenone and estradiol Brand Names in Pakistan:
No Brands Available in Pakistan.