PRODUCT MONOGRAPH. 17β-Estradiol Tablets, USP. 0.5 mg, 1 mg and 2 mg. 17β-Estradiol (as Estradiol Hemihydrate) Estrogen

PRODUCT MONOGRAPH

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LUPIN-ESTRADIOL

17β-Estradiol Tablets, USP 0.5 mg, 1 mg and 2 mg 17β-Estradiol (as Estradiol Hemihydrate) Estrogen

Lupin Phar

Author Karin Potter

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PRODUCT MONOGRAPH

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LUPIN-ESTRADIOL

17β-Estradiol Tablets, USP 0.5 mg, 1 mg and 2 mg 17β-Estradiol (as Estradiol Hemihydrate) Estrogen

Lupin Pharma Canada Limited 1155 René-Lévesque West Blvd., Suite 2500 Montreal, Quebec H3B 2K4 Control No.: 183279

Date of Preparation: 13 November 2015

TABLE OF CONTENTS PART I: HEALTH PROFESSIONAL INFORMATION ........................................................ 3 SUMMARY PRODUCT INFORMATION ............................................................................... 3 INDICATIONS AND CLINICAL USE..................................................................................... 3 CONTRAINDICATIONS .......................................................................................................... 3 WARNINGS AND PRECAUTIONS ........................................................................................ 4 ADVERSE REACTIONS ........................................................................................................ 12 DRUG INTERACTIONS ......................................................................................................... 15 DOSAGE AND ADMINISTRATION ..................................................................................... 16 OVERDOSAGE ....................................................................................................................... 17 ACTION AND CLINICAL PHARMACOLOGY ................................................................... 18 STORAGE AND STABILITY ................................................................................................ 19 DOSAGE FORMS, COMPOSITION AND PACKAGING .................................................... 19 PART II: SCIENTIFIC INFORMATION ............................................................................... 21 PHARMACEUTICAL INFORMATION ................................................................................ 21 CLINICAL TRIALS................................................................................................................. 22 DETAILED PHARMACOLOGY............................................................................................ 25 TOXICOLOGY ........................................................................................................................ 25 REFERENCES ......................................................................................................................... 27 PART III: CONSUMER INFORMATION ............................................................................. 32

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LUPIN-ESTRADIOL (17β-Estradiol Tablets) 0.5 mg, 1 mg and 2 mg 17β-Estradiol (as Estradiol Hemihydrate)

Estrogen PART I: HEALTH PROFESSIONAL INFORMATION SUMMARY PRODUCT INFORMATION Route of Administration Oral

Dosage Form / All Nonmedicinal Ingredients Strength Tablet / 0.5 mg, Lactose monohydrate, corn starch, colloidal silicon 1 mg and 2 mg dioxide, copovidone, magnesium stearate, FD&C Blue No. 1 (1 mg and 2 mg), FD&C Red No. 27 (1 mg), FD&C Yellow No. 5 (2 mg).

INDICATIONS AND CLINICAL USE LUPIN-ESTRADIOL (17β-estradiol) tablets are indicated for: • The symptomatic relief of menopausal symptoms. • LUPIN-ESTRADIOL may also contribute to the prevention of osteoporosis in naturally occurring or surgically induced estrogen-deficiency states when combined with other important therapeutics such as diet, calcium and vitamin D intake, smoking cessation and regular physical weight bearing exercises. The use of LUPIN-ESTRADIOL in the prevention of osteoporosis is to be considered in light of other available therapies. In patients with an intact uterus, LUPIN-ESTRADIOL should always be supplemented by sequential administration of a progestogen in order to prevent endometrial hyperplasia or carcinoma. CONTRAINDICATIONS Estrogen including LUPIN-ESTRADIOL should not be administered to patients with any of the following conditions: • •

Liver dysfunction or disease as long as liver function tests have failed to return to normal. Known or suspected estrogen-dependent malignant neoplasia (e.g., endometrial Page 3 of 36

• • • • • • • • • •

cancer). Endometrial hyperplasia. Known, suspected, or past history of breast cancer. Undiagnosed abnormal genital bleeding. Known or suspected pregnancy. Lactation Active or past history of arterial thromboembolic disease (e.g., stroke, myocardial infarction, coronary heart disease). Classical migraine Active or past history of confirmed venous thromboembolism (such as deep vein thrombosis or pulmonary embolism) or active thrombophlebitis. Partial or complete loss of vision or diplopia, from ophthalmic vascular disease. Hypersensitivity to this drug or to any ingredient in the formulation or component of the container. For a complete listing, see the Dosage Forms, Composition and Packaging section of the Product Monograph.

WARNINGS AND PRECAUTIONS Serious Warnings and Precautions The Women’s Health Initiative (WHI) trial examined the health benefits and risks of combined estrogen plus progestin therapy (n=16,608) and estrogen-alone therapy (n=10,739) in postmenopausal women aged 50 to 79 years.5,40,41 The estrogen plus progestin arm of the WHI trial indicated increased risk of myocardial infarction (MI), stroke, invasive breast cancer, pulmonary emboli and deep vein thrombosis in postmenopausal women receiving treatment with combined conjugated equine estrogens (CEE, 0.625mg/day) and medroxyprogesterone acetate (MPA, 2.5 mg/day) for 5.2 years compared to those receiving placebo.41 The estrogen-alone arm of the WHI trial indicated an increased risk of stroke and deep vein thrombosis in hysterectomized women treated with CEE-alone (0.625 mg/day) for 6.8 years compared to those receiving placebo.40 Therefore, the following should be given serious consideration at the time of prescribing: 1. Estrogens with or without progestins should not be prescribed for primary or secondary prevention of cardiovascular diseases. 2. Estrogens with or without progestins should be prescribed at the lowest effective dose for the approved indication. 3. Estrogens with or without progestins should be prescribed for the shortest period possible for the approved indication. 4. The use of LUPIN-ESTRADIOL for the prevention of osteoporosis should be considered in light of other available therapies.

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Carcinogenesis and Mutagenesis Breast cancer Available epidemiological data indicate that the use of combined estrogen plus progestin by postmenopausal women is associated with an increased risk of invasive breast cancer. In the estrogen plus progestin arm of the WHI trial, among 10,000 women over a one-year period, there were: • 8 more cases of invasive breast cancer [38 on combined hormone replacement therapy (HRT) versus 30 on placebo].41 The WHI study also reported that the invasive breast cancers diagnosed in the estrogen plus progestin group were similar in histology but were larger (mean [SD], 1.7cm [1.1] vs 1.5cm [0.9], respectively; p=0.04) and were at a more advanced stage compared with those diagnosed in the placebo group. The percentage of women with abnormal mammograms (recommendations for short-interval follow-up, a suspicious abnormality, or highly suggestive of malignancy) was significantly higher in the estrogen plus progestin group versus the placebo group. This difference appeared at year one and persisted in each year thereafter.5 In the estrogen-alone arm of the WHI trial, there was no statistically significant difference in the rate of invasive breast cancer in hysterectomized women treated with conjugated equine estrogens versus women treated with placebo.40 In a pivotal clinical study with estradiol (n=64) on the prevention of early post-menopausal bone loss (see Clinical Trials), three (3) abnormal mammograms were reported posttreatment, however, none showed evidence of malignancy. It is recommended that estrogens not be given to women with existing breast cancer or those with a previous history of the disease. There is a need for caution in prescribing estrogens for women with known risk factors associated with the development of breast cancer, such as strong family history of breast cancer (first degree relative) or who present a breast condition with an increased risk (abnormal mammograms and/or atypical hyperplasia at breast biopsy). Other known risk factors for the development of breast cancer such as nulliparity, obesity, early menarche, late age at first full term pregnancy and at menopause should also be evaluated. It is recommended that women undergo mammography prior to the start of HRT treatment and at regular intervals during treatment, as deemed appropriate by the treating physician and according to the perceived risks for each patient.

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The overall benefits and possible risks of hormone replacement therapy should be fully considered and discussed with patients. It is important that the modest increased risk of being diagnosed with breast cancer after 4 years of treatment with combined estrogen plus progestin HRT (as reported in the results of WHI-trial) be discussed with the patient and weighed against its known benefits. Instructions for regular self-examination of the breasts should be included in this counseling. Endometrial hyperplasia & endometrial carcinoma The use of unopposed estrogen by women with intact uteri increases the risk of endometrial hyperplasia and endometrial carcinoma. Estrogen should be prescribed with an appropriate dosage of a progestin in women with intact uteri in order to prevent endometrial hyperplasia/carcinoma. During the conduct of a pivotal clinical study in an open-labeled study of 369 women (mean age = 49) with endogenous estrogen deficiency associated with menopausal symptoms (see Clinical Trials), endometrial biopsies were conducted in a subset of 32 subjects prior to and after therapy. Prior to therapy eleven (11) samples were considered abnormal: cystic hyperplasia (4), adenomatous hyperplasia (6) and mixed-inactive hyperplasia (1). One (1) sample biopsy remained abnormal after 11 months of treatment with estradiol, changing from cystic hyperplasia to benign cystic hyperplasia. In a second pivotal clinical study on the prevention of early post-menopausal bone loss (see Clinical Trials), exit endometrial biopsy specimens were obtained for 21 subjects. Abnormalities consistent with estrogen stimulation of the endometrium were found in 27% of these subjects. Two (2) subjects had progression to the point of adenomatous hyperplasia and one ( 1) subject had atypical nuclear changes. No subjects, however, developed adenocarcinoma of the endometrium. Ovarian cancer Recent epidemiologic studies have found the use of hormone replacement therapy (estrogenalone and estrogen plus progestin therapies), in particular for five or more years, has been associated with an increased risk of ovarian cancer. Cardiovascular The results of the Heart and Estrogen/progestin Replacement Studies (HERS and HERS II) and the WHI trial indicate that the use of estrogen plus progestin is associated with an increased risk of coronary heart disease (CHD) in postmenopausal women.13, 19, 41 The results of the WHI trial indicate that the use of estrogen-alone and estrogen plus progestin is associated with an increased risk of stroke in postmenopausal women.40,41

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WHI trial findings In the combined estrogen plus progestin arm of the WHI trial, among 10,000 women over a one-year period, there were: • 8 more cases of stroke (29 on combined HRT versus 21 on placebo) • 7 more cases of CHD (37 on combined HRT versus 30 on placebo).41 In the estrogen-alone arm of the WHI trial of women with prior hysterectomy, among 10,000 women over a one-year period, there were/was: • 12 more cases of stroke (44 on estrogen-alone therapy versus 32 on placebo) • No statistically significant difference in the rate of CHD.40 HERS and HERS II findings In the HERS study of postmenopausal women with documented heart disease (n=2763, average age 66.7 years), a randomized placebo-controlled clinical trial of secondary prevention of CHD, treatment with 0.625 mg/day oral conjugated equine estrogen (CEE) plus 2.5 mg medroxyprogesterone acetate (MPA) demonstrated no cardiovascular benefit. Specifically, during an average follow-up of 4.1 years, treatment with CEE plus MPA did not reduce the overall rate of CHD events in postmenopausal women with established coronary heart disease. There were more CHD events in the hormone-treated group than in the placebo group in year 1, but not during the subsequent years.19 From the original HERS trial, 2321 women consented to participate in an open-label extension of HERS known as HERS II. Average follow-up in HERS II was an additional 2.7 years, for a total of 6.8 years overall. After 6.8 years, hormone therapy did not reduce the risk of cardiovascular events in women with CHD.13 Blood pressure Women using hormone replacement therapy sometimes experience increased blood pressure. Blood pressure should be monitored with HRT use. Elevation of blood pressure in previously normotensive or hypertensive patients should be investigated and HRT may have to be discontinued.

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Endocrine and Metabolism Glucose and lipid metabolism A worsening of glucose tolerance and lipid metabolism have been observed in a significant percentage of peri- and post-menopausal patients. Therefore, diabetic patients or those with a predisposition to diabetes should be observed closely to detect any alterations in carbohydrate or lipid metabolism, especially in triglyceride blood levels. Women with familial hyperlipidemias need special surveillance. Lipid-lowering measures are recommended additionally, before treatment is started. Women with porphyria need special surveillance. Calcium and phosphorus metabolism Because the prolonged use of estrogens influences the metabolism of calcium and phosphorus, estrogens should be used with caution in patients with metabolic and malignant bone diseases associated with hypercalcemia and in patients with renal insufficiency. Hypothyroidism Patients who require thyroid hormone replacement therapy and who are also taking estrogen should have their thyroid function monitored regularly to assure that thyroid hormone levels remain in an acceptable range (see Drug Interactions, Drug-Laboratory Test Interactions). Genitourinary Vaginal bleeding Abnormal vaginal bleeding, due to its prolongation, irregularity or heaviness, occurring during therapy should prompt appropriate diagnostic measures to rule out the possibility of uterine malignancy and the treatment should be re-evaluated. Uterine leiomyomata Pre-existing uterine leiomyomata may increase in size during estrogen use. Growth, pain or tenderness of uterine leiomyomata requires discontinuation of medication and appropriate investigation. Endometriosis Symptoms and physical findings associated with a previous diagnosis of endometriosis may reappear or become aggravated with estrogen use.

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Hematologic Venous thromboembolism Available epidemiological data indicate that use of estrogen with or without progestin by postmenopausal women is associated with an increased risk of developing venous thromboembolism (VTE). In the estrogen plus progestin arm of the WHI trial, among 10,000 women on combined HRT over a one-year period, there were 18 more cases of VTE, including 8 more cases of pulmonary embolism.41 In the estrogen-alone arm of the WHI trial, among 10,000 women on estrogen therapy over a one-year period, there were 7 more cases of venous thromboembolism, although there was no statistically significant difference in the rate of pulmonary embolism.40 Generally recognized risk factors for VTE include a personal history, a family history (the occurrence of VTE in a direct relative at a relatively early age may indicate genetic predisposition) severe obesity (body mass index >30kg/m2) and systemic lupus erythematosus. The risk of VTE also increases with age and smoking. The risk of VTE may be temporarily increased with prolonged immobilization, major surgery or trauma. In women on HRT, attention should be given to prophylactic measures to prevent VTE following surgery. Also, patients with varicose veins should be closely supervised. The physician should be alert to the earliest manifestations of thrombotic disorders (thrombophlebitis, retinal thrombosis, cerebral embolism and pulmonary embolism). If these occur or are suspected, hormone therapy should be discontinued immediately, given the risks of long-term disability or fatality. If feasible, estrogens should be discontinued at least 4 weeks before major surgery which may be associated with an increased risk of thromboembolism, or during periods of prolonged immobilization. Hepatic/Biliary/Pancreatic Gallbladder diseases A 2- to 4-fold increase in the risk of gallbladder disease requiring surgery in women receiving postmenopausal estrogens has been reported. Jaundice Caution is advised in patients with a history of liver and/or biliary disorders. If cholestatic jaundice develops during treatment, the treatment should be discontinued and appropriate investigations carried out.

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Liver function tests Liver function tests should be done periodically in subjects who are suspected of having hepatic disease. For information on endocrine and liver function tests, see Monitoring and Laboratory Tests. Neurologic Cerebrovascular insufficiency Patients who develop visual disturbances, classical migraine, transient aphasia, paralysis or loss of consciousness should discontinue medication. Patients with a previous history of classical migraine and who develop a recurrence or worsening of migraine symptoms should be reevaluated. Dementia Available epidemiological data indicate that the use of combined estrogen plus progestin in women age 65 and over may increase the risk of developing probable dementia. The Women’s Health Initiative Memory Study (WHIMS), a clinical substudy of the WHI, was designed to assess whether postmenopausal hormone replacement therapy (oral estrogen plus progestin or oral estrogen-alone) reduces the risk of dementia in women aged 65 and over and free of dementia at baseline.34,35 In the estrogen plus progestin arm of the WHIMS (n=4532), women with intact uteri were treated with daily 0.625 mg conjugated equine estrogens (CEE) plus 2.5 mg medroxyprogesterone acetate (MPA) or placebo for an average of 4.05 years. The results, when extrapolated to 10,000 women treated over a one-year period showed: • 23 more cases of probable dementia (45 on combined HRT versus 22 on placebo).34 In the estrogen-alone arm of the WHIMS (n=2947), women with prior hysterectomy were treated with daily 0.625 mg CEE or placebo for an average of 5.21 years. The results, when extrapolated to 10,000 women treated over a one-year period showed: • 12 more cases of probable dementia (37 on estrogen-alone versus 25 on placebo), although this difference did not reach statistical significance.35

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When data from the estrogen plus progestin arm of the WHIMS and the estrogen-alone arm of the WHIMS were combined, as per the original WHIMS protocol, in 10,000 women over a one-year period, there were: •

18 more cases of probable dementia (41 on estrogen plus progestin or estrogen-alone versus 23 on placebo).35

Epilepsy Particular caution is indicated in women with epilepsy, as HRT may cause an exacerbation of this condition. Renal Fluid retention Estrogens may cause fluid retention. Therefore, particular caution is indicated in cardiac or renal dysfunction, epilepsy or asthma. If, in any of the above-mentioned conditions, a worsening of the underlying disease is diagnosed or suspected during treatment, the benefits and risks of treatment should be reassessed based on the individual case. Special Populations Geriatrics (>65 years of age): The use of combined estrogen plus progestin in women aged 65 and over may increase the risk of developing probable dementia (see Warnings and Precautions, Neurologic). Monitoring and Laboratory Tests Before LUPIN-ESTRADIOL is administered, the patient should have a complete physical examination including a blood pressure determination. Breasts and pelvic organs should be appropriately examined and a Papanicolaou smear should be performed. Endometrial biopsy should be done only when indicated. Baseline tests should include mammography, measurements of blood glucose, calcium, triglycerides and cholesterol, and liver function tests. The first follow-up examination should be done within 3-6 months after initiation of treatment to assess response to treatment. Thereafter, examinations should be made at intervals at least once a year. Appropriate investigations should be arranged at regular intervals as determined by the physician. The importance of regular self-examination of the breasts should be discussed with the patient.

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ADVERSE REACTIONS Adverse Drug Reaction Overview See Warnings and Precautions regarding potential induction of malignant neoplasms and adverse effects similar to those of oral contraceptives. The following adverse reactions have been reported with estrogen/progestin combination in general: Blood and lymphatic system disorders Altered coagulation tests (see Warnings and Precaution, Hematologic and Drug Interactions, Drug-Laboratory Test Interactions). Cardiac disorders Increase in blood pressure (see Warnings and Precautions, Cardiovascular); coronary thrombosis; palpitations. Congenital, Familial and Genetic disorders Precipitation or aggravation of porphyria cutanea tarda in predisposed individuals. Endocrine disorders Increased blood sugar levels; decreased glucose tolerance. Eye disorders Intolerance to contact lenses; neuro-ocular lesions (e.g., retinal thrombosis, optic neuritis); steepening of the corneal curvature; visual disturbances. Gastrointestinal disorders Abdominal discomfort (cramps, pressure, pain, bloating); nausea; vomiting. General disorders and administration site conditions Anorexia; changes in appetite; changes in body weight; fatigue; change in libido. Hepatobiliary disorders Asymptomatic impaired liver function; cholestatic jaundice; gallbladder disorder. Musculoskeletal and connective tissue disorders Musculoskeletal pain including leg pain not related to thromboembolic disease (usually transient, lasting 3-6 weeks) may occur. Nervous system disorders Aggravation of migraine episodes; dizziness; headaches; neuritis. Psychiatric disorders Irritability; mental depression; nervousness.

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Renal and urinary disorders Cystitis; dysuria; edema; sodium retention. Reproductive system and breast disorders Breakthrough bleeding; breast swelling, tenderness and secretion; changes in cervical erosion and amount of cervical secretion; change in menstrual flow; dysmenorrhea; dyspareunia; endometrial hyperplasia; increased cervical mucous; increase in size of uterine leiomyomata; pre-menstrual-like syndrome; reactivation of endometriosis; spotting; vaginal candidiasis; vaginal itching/discharge. Skin and subcutaneous tissue disorders Chloasma or melasma, which may persist when drug is discontinued; erythema multiforme; erythema nodosum; hemorrhagic eruption; hirsutism and acne; itching, allergic reactions and rashes; loss of scalp hair; pigmentation of skin Vascular disorders Isolated cases of thromboembolic disorders; thrombophlebitis Clinical Trial Adverse Drug Reactions Because clinical trials are conducted under very specific conditions, the adverse drug reaction rates observed in the clinical trials may not reflect the rates observed in practice and should not be compared to the rates in the clinical trials of another drug. Adverse drug reaction information from clinical trials is useful for identifying drug-related adverse events and for approximating rates. The following table summarizes the adverse events reported in a controlled, randomized, double-blind study with estradiol for the treatment of osteoporosis in 64 post-menopausal women. Estradiol was administered in a cyclic manner for up to 18 months with an option to continue for an additional 6 months.

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Table 1

Reported Adverse Events for More Than One Patient Per Dose Group: Symptoms by Treatment Assignment 0.5 mg estradiol n=15 (%)

1.0 mg estradiol n=16 (%)

2.0 mg estradiol n=16 (%)

Placebo n=16 (%)

2 (13%)

1 (6%)

0

1 (6%)

0

0

0

2 (13%)

0

0

2 (13%)

1 (6%)

3 (20%)

3 (19%)

2 (13%)

1 (6%)

0

0

1 (6%)

2 (13%)

nervousness

1 (7%)

2 (13%)

5 (31%)

2 (13%)

depression

2 (13%)

0

3 (19%)

3 (19%)

insomnia

0

1 (6%)

2 (13%)

2 (13%)

libido decreased

0

0

0

2 (13%)

2 (13%)

1 (6%)

2 (13%)

1 (6%)

menopausal systems1

10 (67%)

11 (69%)

11 (69%)

13 (81%)

vaginal hemorrhage

2 (13%)*

7 (44%)*

9 (56%)*

1 (6%)

1 (7%)

2 (13%)

0

0

0

0

2 (13%)

0

Gastrointestinal Disorders constipation nausea General Disorders & Administration Site Conditions asthenia Investigations weight increased Nervous System Disorders headache Psychiatric Disorders

Renal & Urinary Disorders edema Reproductive System & Breast disorders

vaginitis uterine spasm

* statistically significant at 5% level (Fisher’s exact test) 1 according to MedDRA dictionary, including symptoms such as vasomotor symptoms or hot flushes and vaginal dryness.

If adverse symptoms persist, the prescription of HRT should be reconsidered.

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DRUG INTERACTIONS Overview Estrogens may diminish the effectiveness of anticoagulants, antidiabetic and antihypertensive agents. In vitro and in vivo studies have shown that estrogens are metabolized partially by cytochrome P450 3A4 (CYP 3A4).43-44 Therefore, inducers or inhibitors of CYP 3A4 may affect estrogen drug metabolism. Inducers of CYP 3A4 such as St. John’s Wort (Hypericum perforatum) preparations, phenobarbital, carbamazepine and rifampin may reduce plasma concentrations of estrogens, possibly resulting in a decrease in therapeutic effects and/or changes in uterine bleeding profile. Inhibitors of CYP 3A4 such as erythromycin, clarithromycin, ketoconazole, itraconazole, ritonavir and grapefruit juice may increase plasma concentrations of estrogens and may result in side effects. Other preparations inducing liver enzymes, (e.g., barbiturates, hydantoins, meprobamate or phenylbutazone) may interfere with the activity of orally administered estrogens. One in vitro study has shown cytochrome P450 1A2 (CYP 1A2) to be partially involved in the metabolism of 17β-estradiol through hydroxylation.43-45 The clinical significance of CYP 1A2 metabolism is unknown. Clinical pharmacokinetic studies have not demonstrated any consistent effect of antibiotics (other than rifampin) on plasma concentrations of synthetic steroids. Drug-Drug Interactions Possible drug-drug interactions with estradiol specifically have not been established. Drug-Food Interactions Inhibitors of CYP 3A4 such as grapefruit juice may increase plasma concentrations of estrogens and may result in side effects.47-48 Drug-Herb Interactions It was found that some herbal products (e.g., St. John’s Wort) which are available as over-thecounter (OTC) products might interfere with steroid metabolism and therefore alter the efficacy and safety of estrogen/progestin products. Physicians and other health care providers should be made aware of other non-prescription products concomitantly used by the patient, including herbal and natural products obtained from the widely spread health stores.

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Drug-Laboratory Test Interactions The results of certain endocrine and liver function tests may be affected by estrogencontaining products. • Increased prothrombin time and partial thromboplastin time; increased levels of fibrinogen and fibrinogen activity; increased coagulation factors VII, VIII, IX, X; • Decreased antithrombin III (although following administration of estradiol for 28 days no effect on antithrombin III levels was seen); increased norepinephrine-induced platelet aggregability; • Increased thyroxine-binding globulin (TBG) (although TBG was not affected in clinical trials with estradiol), leading to increased circulating total thyroid hormone (T4) as measured by column or radioimmunoassay; T3 resin uptake is decreased, reflecting the elevated TBG, free T4 concentration is unaltered. • Other binding proteins may be elevated in serum i.e. corticosteroid binding globulin (CBG), sex-hormone binding globulin (SHBG), leading to increased circulating corticosteroids and sex steroids respectively; free or biologically active hormone concentrations are unchanged; • Reduced serum folate concentration; • Increased serum triglyceride and phospholipid concentrations; • Impaired glucose tolerance. The results of the above laboratory tests should not be considered reliable unless therapy has been discontinued for two to four weeks. The pathologist should be informed that the patient is receiving HRT when relevant specimens are submitted. Drug-Lifestyle Interactions The effect of lifestyle choices (e.g., smoking) on the use of estradiol has not been established. DOSAGE AND ADMINISTRATION Dosing Considerations The lowest dose of estrogen required to prevent menopausal symptoms and to prevent development of osteoporosis should be used. LUPIN-ESTRADIOL should be taken at the same time each day.

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Recommended Dose and Dosage Adjustment In general, estrogen is usually administered cyclically for the first 21 to 25 days of each month. In patients with intact uteri, a progestin should be sequentially administered for the last 12 to 14 days of estrogen administration in order to prevent development of endometrial hyperplasia/carcinoma as a result of estrogen stimulation. In hysterectomized patients, estrogen alone should be given continuously. Menopausal symptoms: Treatment of menopausal symptoms is usually initiated with 1 mg LUPIN-ESTRADIOL tablet per day. Thereafter, the dosage should be adjusted to the needs of the individual. Attempts to taper or discontinue the medication should be made at 3 to 6 month intervals. For prevention of osteoporosis: Prophylactic therapy with LUPIN-ESTRADIOL to prevent postmenopausal bone loss should be initiated with 0.5 mg LUPIN-ESTRADIOL tablet per day as soon as possible after menopause. The dose may be titrated upward and downward based on the patient’s clinical status and plasma estradiol levels. Ideally, plasma estradiol levels should be maintained around 50 pg/mL. Missed Dose LUPIN-ESTRADIOL should be taken as soon as possible after missing a dose. However the missed dose should be skipped if it is almost time to take the next dose. Patients should be advised not to double the dose. OVERDOSAGE Symptoms Numerous reports of ingestion of large doses of estrogen products and estrogen-containing oral contraceptives by young children have not revealed acute serious ill effects. Overdosage with estrogen may cause nausea, breast discomfort, fluid retention, bloating or vaginal bleeding in women. Treatment Remove ingested drug by gastric lavage and give symptomatic treatment. For management of a suspected drug overdose, contact your regional Poison Control Centre.

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ACTION AND CLINICAL PHARMACOLOGY Mechanism of Action Estradiol is the most potent physiologic estrogen and, in fact, is the major estrogenic hormone secreted in humans. Estradiol controls the development and maintenance of the female sex organs, the secondary sex characteristics and the mammary glands as well as certain functions of the human uterus and accessory organs, particularly the proliferation of the endometrium, the development of the decidua, and the cyclic changes in the cervix and vagina. The production of estradiol by the ovaries is under the control of pituitary gonadotropins, follicle stimulating hormone (FSH) and luteinizing hormone (LH). In menopausal women, the depletion of ovarian follicles leads to lower plasma estradiol and elevated plasma FSH and LH. Pharmacodynamics The active ingredient in LUPIN-ESTRADIOL tablets contain, 17β-estradiol, which is structurally identical to the estradiol produced by the human ovary. Estrogens are secreted mainly by the gonads and in a very small amount by the adrenals. In addition, they are formed, to an important degree, from peripheral conversion of adrenal and gonadal androgens to estrogens. Estradiol is the most potent of the known naturally occurring estrogens in stimulating the growth of the reproductive tissues. Estradiol promotes uterine growth in the rat without undergoing chemical transformation and responsive tissues, such as the uterus and vagina, show a characteristic affinity for estradiol. Estrogen deficiency is manifested by hot flushes, sweating, insomnia, paresthesia, irritability, and urogenital atrophy. As replacement therapy in estrogen deficiency states (such as menopause), low doses of estradiol in cyclic regimens have been found to relieve such deficiency. Estrogen deficiency is the main cause of postmenopausal bone loss and contributes to age-associated losses leading to osteoporosis. Numerous clinical studies have demonstrated that estrogen therapy prevents bone loss and reduces the incidence of vertebral, hip, and Colles’ fractures. Although the mechanism of action of estrogen on bone metabolism is still not completely elucidated, estrogens have been shown to have several effects: increase in renal tubular absorption of calcium, thus reducing urinary calcium; decrease in the sensitivity of bone to the parathyroid hormone (PTH); increase in the intestinal absorption of calcium and increase in circulating levels of active 1-25-dihydroxyvitamin D. Recent research has shown that osteoblasts also possess receptors for estrogens.

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Pharmacokinetics A number of steroids with 3 oxygen functions have been identified such as 16-epiestriol, 16-ketoestradiol, 16-hydroxyestrone and 2-methoxyestrone with estradiol being a precursor to these compounds. Absorption: Micronized 17β-estradiol is efficiently absorbed by the gastrointestinal tract.49 The drug passes through the gastrointestinal mucosa and directly into the liver via the portal circulation before its access by the systemic circulation.50 Distribution: Estrogens circulate in both unconjugated and conjugated forms in the blood, with the unconjugated estrogens, either free or bound to proteins, mainly albumin, or to the specific sex-hormone binding globulin (SHBG) which shows a great affinity for estradiol. Metabolism: Estrogens are metabolized mainly in the liver, with the metabolites being conjugated with glucuronic acid or sulfuric acid and even double conjugates such as estriol-3-sulfate-16%-glucuronide are formed. About 1/3 to 1/2 of the circulating estrogens are secreted in the bile and of this fraction 20% is reabsorbed after hydrolysis in the intestinal tract. The exact site of the hydrolysis is not known, but it probably takes place in the intestinal lumen and is catalyzed by enzymes secreted into the intestinal tract or present in the microflora. Excretion: When administered to humans, about 65% of the dose is excreted in the urine, almost entirely in the water-soluble form as β-glucuronides or sulfate esters. Estrone, estradiol and estriol account for about 1/2 of the excreted products. STORAGE AND STABILITY Store at room temperature (15°C-30°C). Keep container tightly closed and protect from light. DOSAGE FORMS, COMPOSITION AND PACKAGING LUPIN-ESTRADIOL tablets are taken orally. LUPIN-ESTRADIOL 0.5mg: Each tablet contains 0.5 mg of micronized 17β-estradiol (as estradiol hemihydrate). Nonmedicinal ingredients: corn starch, colloidal silicon dioxide, copovidone, lactose monohydrate, magnesium stearate. Tablet is white to off-white, round shaped tablet debossed with “E5” on one side and scored on the other side. LUPIN-ESTRADIOL 1 mg: Each tablet contains 1 mg of micronized 17β-estradiol (as estradiol hemihydrate). Nonmedicinal ingredients: corn starch, colloidal silicon dioxide, copovidone, lactose monohydrate, magnesium stearate, FD&C Blue No. 1, FD&C Red No. 27. Tablet is lavender, mottled, round shaped tablet debossed with “E1” on one side and scored on the other side.

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LUPIN-ESTRADIOL 2 mg: Each tablet contains 2 mg of micronized 17β-estradiol (as estradiol hemihydrate). Nonmedicinal ingredients: corn starch, colloidal silicon dioxide, copovidone, lactose monohydrate, magnesium stearate, FD&C Blue No. 1, FD&C Yellow No. 5. Tablet is turquoise, mottled, round shaped tablet debossed with “E2” on one side and scored on the other side. LUPIN-ESTRADIOL tablets are available as round shaped compressed tablets containing 17βestradiol (as estradiol hemihydrate) in bottles of 100.

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PART II: SCIENTIFIC INFORMATION PHARMACEUTICAL INFORMATION Drug Substance Proper name:

Estradiol Hemihydrate

Chemical name:

Estra-1,3,5(10)-triene-3,17β-diol

Molecular formula and molecular mass:

C18H24O2•½ H2O

281.4 g/mol

Structural formula:

Physicochemical properties: Estradiol is a white odorless crystalline solid, with a melting range of 173°-179°C. It is practically insoluble in water, freely soluble in alcohol, soluble in acetone, dioxane, chloroform, in solutions of fixed alkali hydroxides and sparingly soluble in vegetable oils.

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CLINICAL TRIALS Comparative Bioavailability: A single dose oral bioavailability study of LUPIN-ESTRADIOL (17β-estradiol) 2.0 mg tablets (Lupin Pharma Canada Ltd.) was performed against ESTRACE (17β-estradiol) 2.0 mg tablets in 46 healthy post-menopausal female subjects under fasting conditions. Results of the study are summarized below. SUMMARY TABLE OF THE COMPARATIVE BIOAVAILABILITY DATA 17β-Estradiol (1 x 2 mg) From measured data Geometric Mean Arithmetic Mean (CV %) Test*

Parameter

Reference†

% Ratio of Geometric Means 97.13

90% Confidence Interval

AUCT 1556.80 1604.73 91.79 to 102.79 (pg*hr/mL) 1656.83 (37.29) 1720.66 (39.24) AUCI 1655.72 1669.69 99.26 94.74 to 104.00 (pg*hr/mL) 1774.33 (40.00) 1782.13 (37.03) Cmax 62.82 62.18 101.33 93.54 to 109.76 (pg/mL) 68.88 (51.97) 67.55 (41.73) Tmax§ 5.06 7.17 (h) 7.19 (56.18) 8.59 (49.08) T ½€ 14.69 14.94 (h) 15.52 (34.91) 15.81 (31.55) * Test product - LUPIN-ESTRADIOL as marketed by Lupin Pharma Canada Limited, Canada. † Reference product – ESTRACE (17β-estradiol) by Shire Canada Inc. (purchased in Canada). This product is currently marketed by Acerus Pharmaceuticals Corporation. § Expressed as the arithmetic mean (CV%) only € Expressed as the arithmetic mean (CV%) only

Efficacy and Safety Studies Study demographics and trial design Table 2 Study #

139

Summary of Patient Demographics for Clinical Trials in Specific Indication Trial design

Open-label

Dosage, route of administration and duration 1mg/day 1,* or 2mg/day2,*, orally (21 of 28 day cyclic regimen). Titration up to 4mg/day. Duration up to a year.

Study subjects (n=number)

Mean age

Gender

369

49 years

Female

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Table 2

Summary of Patient Demographics for Clinical Trials in Specific Indication

Study #

7092

Trial design

Randomized, doubleblind, placebocontrolled, parallel group

Dosage, route of administration and duration

Study subjects (n=number)

Mean age

Gender

Placebo, 0.5mg, 1mg or 2mg/day. 18 months with an option of continuing another 6 months.

64

52.8 years

Female

(Range: 42-58)

1. Subjects with up to 5 hot flashes per day. 2. Subjects with more than 5 hot flashes per day. * Dose titrated to a maximum of 4 mg/day for those not relieved by initial doses.

The safety and efficacy of estradiol in alleviating menopausal symptoms was evaluated in an open-label study (#139) of 369 women with endogenous estrogen deficiency associated with menopausal symptoms (Table 2). The safety and efficacy of estradiol in preventing early post-menopausal bone loss was evaluated in a randomized, double-blind, placebo-controlled, parallel group, dose-ranging clinical study (#7092). Sixty-four (64) subjects with natural or surgical menopause were randomly assigned to one of 4 treatment groups: placebo (17), estradiol 0.5 mg (15), 1 mg (16) or 2 mg (16) (Table 2). Treatment was administered as a 23 of 28 day cyclic regimen for a period of up to 18 months with an option to continue for an additional 6 months. All groups were supplemented with calcium tablets up to a total of 1500 mg elemental calcium daily. Study results Symptomatic relief of menopausal symptoms Table 3

Results of Study # 139 Alleviating Menopausal Symptoms

Primary Endpoints

Associated value and statistical significance for Drug at specific dosages

Associated value and statistical significance for Placebo or active control

Relief from hot flashes

At doses of 1 to 4mg/day, estradiol provided relief of hot flashes in 95.6% of the subjects

Not applicable because there was no placebo or active control group.

In study #139, one hundred (100) subjects (27.1%) were on treatment from 0-4 months while 269 (72.9%) were treated for more than 4 months and up to more than one year for 48 patients (13.0%). Fifty-five (55) subjects dropped out of the study due to persistent menopausal symptoms (14), side effects (7), bleeding problem (1) or other reasons not related to treatment (33). Overall, estradiol provided relief of hot flashes for 305 (95.6%) subjects (Table 3). Of the 319 subjects evaluated for efficacy, 77.4% were relieved of their symptoms with the initial

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dosage of 1 or 2 mg, and 22.6% required a change to the initial dosage. In total, 8.1% of the subjects required dose increases up to 3 or 4 mg. Other menopausal symptoms such as sweating, tingling, and genital atrophy were reported by 54%, 22% and 17% of the subjects, respectively. At the end of the study, only 11% of all patients reported having any of these symptoms. The most commonly reported side effects during the course of the study were edema (29%), breast soreness (22%), uterine bleeding (7%) and weight gain (4%). Patients also complained of menopausal symptoms such as depression (36%), headache (19%), insomnia (18%), fatigue (13%) and decreased libido (6%). In conclusion, estradiol at doses of 1 to 4 mg/day given in a 21 of 28 day cyclic regimen was safe and efficacious for the treatment of symptoms related to endogenous estrogen deficiency. Prevention of osteoporosis Table 4

Results of Study # 7092 Prevention of Bone Loss

Primary Endpoints

Associated value and statistical significance for Drug at specific dosages

Associated value and statistical significance for Placebo or active control

Measurement of bone mineral density (n=45)

Non statistically significant trend found for increase in mean adjusted annual bone density at 0.5 mg, 1 mg or 2 mg (0.2%, 1.9% and 1.0% respectively)

5.7% mean adjusted annual bone loss in Placebo group (p

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