DEPO-PROVERA - medroxyprogesterone acetate injection, suspension
DEPO-PROVERA - medroxyprogesterone acetate injection, suspension
Pharmacia and Upjohn Company
DEPO-PROVERA®
Contraceptive Injection
medroxyprogesterone acetate injectable suspension, USP
Physician Information
Women who use Depo-Provera Contraceptive Injection may lose significant bone mineral density. Bone loss is greater with increasing duration of use and may not be completely reversible.
It is unknown if use of Depo-Provera Contraceptive Injection during adolescence or early adulthood, a critical period of bone accretion, will reduce peak bone mass and increase the risk for osteoporotic fracture in later life.
Depo-Provera Contraceptive Injection should be used as a long-term birth control method (e.g. longer than 2 years) only if other birth control methods are inadequate. (See WARNINGS.)
Patients should be counseled that this product does not protect against HIV infection (AIDS) and other sexually transmitted diseases.
DESCRIPTION
DEPO-PROVERA Contraceptive Injection (CI) contains medroxyprogesterone acetate, a derivative of progesterone, as its active ingredient. Medroxyprogesterone acetate is active by the parenteral and oral routes of administration. It is a white to off-white; odorless crystalline powder that is stable in air and that melts between 200°C and 210°C. It is freely soluble in chloroform, soluble in acetone and dioxane, sparingly soluble in alcohol and methanol, slightly soluble in ether, and insoluble in water.
The chemical name for medroxyprogesterone acetate is pregn-4-ene-3,20-dione, 17-(acetyloxy)-6-methyl-, (6α-).
The structural formula is as follows:
DEPO-PROVERA CI for intramuscular (IM) injection is available in vials and prefilled syringes, each containing 1 mL of medroxyprogesterone acetate sterile aqueous suspension 150 mg/mL.
Each mL contains:
|
Medroxyprogesterone acetate |
150 mg |
|
Polyethylene glycol 3350 |
28.9 mg |
|
Polysorbate 80 |
2.41 mg |
|
Sodium chloride |
8.68 mg |
|
Methylparaben |
1.37 mg |
|
Propylparaben |
0.150 mg |
|
Water for injection |
qs |
When necessary, pH is adjusted with sodium hydroxide or hydrochloric acid, or both.
CLINICAL PHARMACOLOGY
DEPO-PROVERA CI (medroxyprogesterone acetate), when administered at the recommended dose to women every 3 months, inhibits the secretion of gonadotropins which, in turn, prevents follicular maturation and ovulation and results in endometrial thinning. These actions produce its contraceptive effect.
Following a single 150 mg IM dose of DEPO-PROVERA Contraceptive Injection, medroxyprogesterone acetate concentrations, measured by an extracted radioimmunoassay procedure, increase for approximately 3 weeks to reach peak plasma concentrations of 1 to 7 ng/mL. The levels then decrease exponentially until they become undetectable (<100 pg/mL) between 120 to 200 days following injection. Using an unextracted radioimmunoassay procedure for the assay of medroxyprogesterone acetate in serum, the apparent half-life for medroxyprogesterone acetate following IM administration of DEPO-PROVERA Contraceptive Injection is approximately 50 days.
Women with lower body weights conceive sooner than women with higher body weights after discontinuing DEPO-PROVERA Contraceptive Injection.
The effect of hepatic and/or renal disease on the pharmacokinetics of DEPO-PROVERA Contraceptive Injection is unknown.
INDICATIONS AND USAGE
DEPO-PROVERA CI is indicated only for the prevention of pregnancy. The loss of bone mineral density (BMD) in women of all ages and the impact on peak bone mass in adolescents should be considered, along with the decrease in BMD that occurs during pregnancy and/or lactation, in the risk/benefit assessment for women who use Depo-Provera CI long-term (see WARNINGS.) It is a long-term injectable contraceptive in women when administered at 3-month (13-week) intervals. Dosage does not need to be adjusted for body weight.
In five clinical studies using DEPO-PROVERA CI, the 12-month failure rate for the group of women treated with DEPO-PROVERA CI was zero (no pregnancies reported) to 0.7 by Life-Table method. Pregnancy rates with contraceptive measures are typically reported for only the first year of use as shown in Table 1. Except for intrauterine devices (IUD), implants, sterilization, and DEPO-PROVERA CI, the efficacy of these contraceptive measures depends in part on the reliability of use. The effectiveness of DEPO-PROVERA CI is dependent on the patient returning every 3 months (13 weeks) for reinjection.
Table 1 Lowest Expected and Typical Failure Rates* Expressed as Percent of Women Experiencing an Accidental Pregnancy in the First Year of Continuous Use
|
Method |
Lowest Expected |
Typical |
|
Source: Trussell et al1 |
|
|
|
Injectable progestogen |
|
|
|
DEPO-PROVERA |
0.3 |
0.3 |
|
Implants |
|
|
|
Norplant (6 capsules) |
0.2† |
0.2† |
|
Female sterilization |
0.2 |
0.4 |
|
Male sterilization |
0.1 |
0.15 |
|
Pill |
|
3 |
|
Combined |
0.1 |
|
|
Progestogen only |
0.5 |
|
|
IUD |
|
3 |
|
Progestasert |
2 |
|
|
Copper T 380A |
0.8 |
|
|
Condom |
2 |
12 |
|
Diaphragm |
6 |
18 |
|
Cap |
6 |
18 |
|
Spermicides |
3 |
21 |
|
Sponge |
|
|
|
Parous women |
9 |
28 |
|
Nulliparous women |
6 |
18 |
|
Periodic abstinence |
1–9 |
20 |
|
Withdrawal |
4 |
18 |
|
No method |
85 |
85 |
CONTRAINDICATIONS
-
Known or suspected pregnancy or as a diagnostic test for pregnancy.
-
Undiagnosed vaginal bleeding.
-
Known or suspected malignancy of breast.
-
Active thrombophlebitis, or current or past history of thromboembolic disorders, or cerebral vascular disease.
-
Significant liver disease.
-
Known hypersensitivity to DEPO-PROVERA CI (medroxyprogesterone acetate or any of its other ingredients).
WARNINGS
1. Loss of Bone Mineral Density
Use of Depo-Provera CI reduces serum estrogen levels and is associated with significant loss of bone mineral density (BMD) as bone metabolism accommodates to a lower estrogen level. This loss of BMD is of particular concern during adolescence and early adulthood, a critical period of bone accretion. It is unknown if use of Depo-Provera CI by younger women will reduce peak bone mass and increase the risk for osteoporotic fracture in later life. In both adults and adolescents, the decrease in BMD appears to be at least partially reversible after Depo-Provera CI is discontinued and ovarian estrogen production increases. A study to assess the reversibility of loss of BMD in adolescents is ongoing.
Depo-Provera CI should be used as a long-term birth control method (e.g. longer than 2 years) only if other birth control methods are inadequate. BMD should be eva luated when a woman needs to continue to use Depo-Provera CI long term. In adolescents, interpretation of BMD results should take into account patient age and skeletal maturity.
Other birth control methods should be considered in the risk/benefit analysis for the use of Depo-Provera CI in women with osteoporosis risk factors. Depo-Provera CI can pose an additional risk in patients with risk factors for osteoporosis (e.g., metabolic bone disease, chronic alcohol and/or tobacco use, anorexia nervosa, strong family history of osteoporosis or chronic use of drugs that can reduce bone mass such as anticonvulsants or corticosteroids). Although there are no studies addressing whether calcium and Vitamin D may lessen BMD loss in women using Depo-Provera CI, all patients should have adequate calcium and Vitamin D intake.
BMD Changes in Adult Women
In a controlled, clinical study, adult women using Depo-Provera CI for up to 5 years showed spine and hip BMD mean decreases of 5–6%, compared to no significant change in BMD in the control group. The decline in BMD was more pronounced during the first two years of use, with smaller declines in subsequent years. Mean changes in lumbar spine BMD of −2.86%, -4.11%, -4.89%, -4.93% and −5.38% after 1, 2, 3, 4, and 5 years, respectively, were observed. Mean decreases in BMD of the total hip and femoral neck were similar.
After stopping use of Depo-Provera CI (150 mg), there was partial recovery of BMD toward baseline values during the 2-year post-therapy period. Longer duration of treatment was associated with less complete recovery during this 2-year period following the last injection. Table 2 shows the extent of recovery of BMD for women who completed 5 years of treatment.
Table 2. Mean Percent Change from Baseline in BMD in Adults by Skeletal Site and Cohort
|
Time in Study |
Spine |
Total Hip |
Femoral Neck |
|
|
Depo-Provera* |
Control† |
Depo-Provera* |
Control† |
Depo-Provera* |
Control† |
|
|
|
5 years |
n=33 |
n=105 |
n=21 |
n=65 |
n=34 |
n=106 |
|
|
-5.38% |
0.43% |
-5.16% |
0.19% |
-6.12% |
-0.27% |
|
7 years |
n=12 |
n=60 |
n=7 |
n=39 |
n=13 |
n=63 |
|
|
-3.13% |
0.53% |
-1.34% |
0.94% |
-5.38% |
-0.11% |
BMD Changes in Adolescent Females (12–18 years of age)
Preliminary results from an ongoing, open-label, self-selected, non-randomized clinical study of adolescent females (12–18 years) also showed that Depo-Provera CI use was associated with a significant decline in BMD from baseline (Table 3). In general, adolescents increase bone density during the period of growth following menarche, as seen in the untreated cohort. However, the two cohorts were not matched at baseline for age, gynecologic age, race, BMD and other factors that influence the rate of acquisition of bone mineral density, with the result that they differed with respect to these demographic factors.
Preliminary data from the small number of adolescents participating in the 2-year post-use observation period demonstrated partial recovery of BMD.
Table 3. Mean Percent Change from Baseline in BMD in Adolescents by Skeletal Site and Cohort
|
Duration of Treatment |
Depo-Provera CI
(150 mg IM) |
Unmatched, Untreated
Cohort |
|
|
N |
Mean % Change |
N |
Mean % Change |
|
Total Hip BMD |
|
|
|
|
|
Week 60 (1.2 years) |
103 |
-2.82 |
171 |
1.32 |
|
Week 144 (2.8 years) |
45 |
-6.16 |
111 |
1.74 |
|
Week 240 (4.6 years) |
9 |
-6.92 |
69 |
1.12 |
|
Femoral Neck BMD |
|
|
|
|
|
Week 60 |
103 |
-3.05 |
171 |
1.87 |
|
Week 144 |
45 |
-6.01 |
111 |
2.54 |
|
Week 240 |
9 |
-6.06 |
69 |
1.45 |
|
Lumbar Spine BMD |
|
|
|
|
|
Week 60 |
104 |
-2.42 |
171 |
3.47 |
|
Week 144 |
46 |
-2.78 |
111 |
5.41 |
|
Week 240 |
9 |
-4.17 |
70 |
5.12 |
2. Bleeding Irregularities
Most women using DEPO-PROVERA CI experience disruption of menstrual bleeding patterns. Altered menstrual bleeding patterns include irregular or unpredictable bleeding or spotting, or rarely, heavy or continuous bleeding. If abnormal bleeding persists or is severe, appropriate investigation should be instituted to rule out the possibility of organic pathology, and appropriate treatment should be instituted when necessary.
As women continue using DEPO-PROVERA CI, fewer experience irregular bleeding and more experience amenorrhea. By month 12 amenorrhea was reported by 55% of women, and by month 24 amenorrhea was reported by 68% of women using DEPO-PROVERA CI.2
3. Cancer Risks
Long-term case-controlled surveillance of users of DEPO-PROVERA CI found slight or no increased overall risk of breast cancer3 and no overall increased risk of ovarian,4 liver,5 or cervical6 cancer and a prolonged, protective effect of reducing the risk of endometrial7 cancer in the population of users.
A pooled analysis14 from two case-control studies, the World Health Organization Study3 and the New Zealand Study13, reported the relative risk (RR) of breast cancer for women who had ever used DEPO-PROVERA CI as 1.1 (95% confidence interval (CI) 0.97 to 1.4). Overall, there was no increase in risk with increasing duration of use of DEPO-PROVERA CI. The RR of breast cancer for women of all ages who had initiated use of DEPO-PROVERA CI within the previous 5 years was estimated to be 2.0 (95% CI 1.5 to 2.8).
The World Health Organization Study3, a component of the pooled analysis14 described above, showed an increased RR of 2.19 (95% CI 1.23 to 3.89) of breast cancer associated with use of DEPO-PROVERA CI in women whose first exposure to drug was within the previous 4 years and who were under 35 years of age. However, the overall RR for ever-users of DEPO-PROVERA CI was only 1.2 (95% CI 0.96 to 1.52).
[NOTE: A RR of 1.0 indicates neither an increased nor a decreased risk of cancer associated with the use of the drug, relative to no use of the drug. In the case of the subpopulation with a RR of 2.19, the 95% CI is fairly wide and does not include the value of 1.0, thus inferring an increased risk of breast cancer in the defined subgroup relative to nonusers. The value of 2.19 means that women whose first exposure to drug was within the previous 4 years and who are under 35 years of age have a 2.19 fold (95% CI 1.23 to 3.89-fold) increased risk of breast cancer relative to nonusers. The National Cancer Institute8 reports an average annual incidence rate for breast cancer for US women, all races, age 30 to 34 years of 26.7 per 100,000. A RR of 2.19, thus, increases the possible risk from 26.7 to 58.5 cases per 100,000 women. The attributable risk, thus, is 31.8 per 100,000 women per year.]
A statistically insignificant increase in RR estimates of invasive squamous-cell cervical cancer has been associated with the use of DEPO-PROVERA CI in women who were first exposed before the age of 35 years (RR 1.22 to 1.28 and 95% CI 0.93 to 1.70). The overall, nonsignificant relative rate of invasive squamous-cell cervical cancer in women who ever used DEPO-PROVERA CI was estimated to be 1.11 (95% CI 0.96 to 1.29). No trends in risk with duration of use or times since initial or most recent exposure were observed.
4. Thromboembolic Disorders
The physician should be alert to the earliest manifestations of thrombotic disorders (thrombophlebitis, pulmonary embolism, cerebrovascular disorders, and retinal thrombosis). Should any of these occur or be suspected, the drug should not be readministered.
5. Ocular Disorders
Medication should not be readministered pending examination if there is a sudden partial or complete loss of vision or if there is a sudden onset of proptosis, diplopia, or migraine. If examination reveals papilled
