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Medroxyprogesterone acetate
Clinical data
Pronunciation/mɛˌdrɒksiprˈɛstərn ˈæsɪtt/ me-DROKS-ee-proh-JES-tər-ohn ASS-i-tayt[1]
Trade namesDepo-Provera, others
Other namesMPA; DMPA; Methylhydroxyprogesterone acetate; Methylacetoxyprogesterone; MAP; Methypregnone; Metipregnone; 6α-Methyl-17α-hydroxyprogesterone acetate; 6α-Methyl-17α-acetoxyprogesterone; 6α-Methyl-17α-hydroxypregn-4-ene-3,20-dione acetate; NSC-26386
AHFS/Drugs.comMonograph
MedlinePlusa604039
Pregnancy
category
  • AU: D
Routes of
administration		By mouth, sublingual, intramuscular injection, subcutaneous injection
Drug classProgestogen; Progestin; Progestogen ester; Antigonadotropin; Steroidal antiandrogen
ATC code
Legal status
Legal status
Pharmacokinetic data
BioavailabilityBy mouth: ~100%[3][4]
Protein binding88% (to albumin)[4]
MetabolismLiver (hydroxylation (CYP3A4), reduction, conjugation)[5][3][8]
Elimination half-lifeBy mouth: 12–33 hours[5][3]
IM (aq. susp.Tooltip aqueous suspension): ~50 days[6]
SC (aq. susp.): ~40 days[7]
ExcretionUrine (as conjugates)[5]
Identifiers
  • [(6S,8R,9S,10R,13S,14S,17R)-17-acetyl-6,10,13-trimethyl-3-oxo-2,6,7,8,9,11,12,14,15,16-decahydro-1H-cyclopenta[a]phenanthren-17-yl] acetate
CAS Number
PubChem CID
IUPHAR/BPS
DrugBank
ChemSpider
UNII
KEGG
ChEBI
ChEMBL
CompTox Dashboard (EPA)
ECHA InfoCard100.000.689 Edit this at Wikidata
Chemical and physical data
FormulaC24H34O4
Molar mass386.532 g·mol−1
3D model (JSmol)
Melting point207 to 209 °C (405 to 408 °F)
  • C[C@H]1C[C@@H]2[C@H](CC[C@]3([C@H]2CC[C@@]3(C(=O)C)OC(=O)C)C)[C@@]4(C1=CC(=O)CC4)C
  • InChI=InChI=1S/C24H34O4/c1-14-12-18-19(22(4)9-6-17(27)13-21(14)22)7-10-23(5)20(18)8-11-24(23,15(2)25)28-16(3)26/h13-14,18-20H,6-12H2,1-5H3/t14-,18+,19-,20-,22+,23-,24-/m0/s1
  • Key:PSGAAPLEWMOORI-PEINSRQWSA-N
  (verify)

Medroxyprogesterone acetate (MPA), also known as depot medroxyprogesterone acetate (DMPA) in injectable form and sold under the brand name Depo-Provera among others, is a hormonal medication of the progestin type.[9][3] It is used as a method of birth control and as a part of menopausal hormone therapy.[9][3] It is also used to treat endometriosis, abnormal uterine bleeding, paraphilia, and certain types of cancer.[9] The medication is available both alone and in combination with an estrogen.[10][11] It is taken by mouth, used under the tongue, or by injection into a muscle or fat.[9]

Common side effects include menstrual disturbances such as absence of periods, abdominal pain, and headaches.[9] More serious side effects include bone loss, blood clots, allergic reactions, and liver problems.[9] Use is not recommended during pregnancy as it may harm the baby.[9] MPA is an artificial progestogen, and as such activates the progesterone receptor, the biological target of progesterone.[3] It also has androgenic activity and weak glucocorticoid activity. Due to its progestogenic activity, MPA decreases the body's release of gonadotropins and can suppress sex hormone levels.[12] It works as a form of birth control by preventing ovulation.[9]

MPA was discovered in 1956 and was introduced for medical use in the United States in 1959.[13][14][9] It is on the World Health Organization's List of Essential Medicines.[15] MPA is the most widely used progestin in menopausal hormone therapy and in progestogen-only birth control.[16][17] DMPA is approved for use as a form of long-acting birth control in more than 100 countries.[18][19] In 2023, it was the 257th most commonly prescribed medication in the United States, with more than 1 million prescriptions.[20][21]

Medical uses

[edit]

The most common use of MPA is in the form of DMPA as a long-acting progestogen-only injectable contraceptive to prevent pregnancy in women. It is an extremely effective contraceptive when used with relatively high doses to prevent ovulation. MPA is also used in combination with an estrogen in menopausal hormone therapy in postmenopausal women to treat and prevent menopausal symptoms such as hot flashes, vaginal atrophy, and osteoporosis.[3] It is used in menopausal hormone therapy specifically to prevent endometrial hyperplasia and cancer that would otherwise be induced by prolonged unopposed estrogen therapy in women with intact uteruses.[3][22] In addition to contraception and menopausal hormone therapy, MPA is used in the treatment of gynecological and menstrual disorders such as dysmenorrhea, amenorrhea, and endometriosis.[23] Along with other progestins, MPA was developed to allow for oral progestogen therapy, as progesterone (the progestogen hormone made by the human body) could not be taken orally for many decades before the process of micronization was developed and became feasible in terms of pharmaceutical manufacturing.[24]

DMPA reduces sex drive in men and is used as a form of chemical castration to control inappropriate or unwanted sexual behavior in those with paraphilias or hypersexuality, including in convicted sex offenders.[25][26] DMPA has also been used to treat benign prostatic hyperplasia, as a palliative appetite stimulant for cancer patients, and at high doses (800 mg per day) to treat certain hormone-dependent cancers including endometrial cancer, renal cancer, and breast cancer.[27][28][29][30][31] MPA has also been prescribed in feminizing hormone therapy for transgender women due to its progestogenic and functional antiandrogenic effects.[32] It has been used to delay puberty in children with precocious puberty but is not satisfactory for this purpose as it is not able to completely suppress puberty (specifically, it does not fully halt skeletal maturation and hence does not sufficiently resolve the reduced height at adulthood).[33] DMPA at high doses has been reported to be definitively effective in the treatment of hirsutism as well.[34]

Though not used as a treatment for epilepsy, MPA has been found to reduce the frequency of seizures and does not interact with antiepileptic medications. MPA does not interfere with blood clotting and appears to improve blood parameters for women with sickle cell anemia. Similarly, MPA does not appear to affect liver metabolism, and may improve primary biliary cirrhosis and chronic active hepatitis. Women taking MPA may experience spotting shortly after starting the medication but is not usually serious enough to require medical intervention. With longer use amenorrhea (absence of menstruation) can occur as can irregular menstruation which is a major source of dissatisfaction, though both can result in improvements with iron deficiency and risk of pelvic inflammatory disease and often do not result in discontinuation of the medication.[28]

Birth control

[edit]
Depot medroxyprogesterone acetate (DMPA)
Background
TypeHormonal
First use1969[35]
Trade namesDepo-Provera, Depo-SubQ Provera 104, others
AHFS/Drugs.comdepo-provera
Failure rates (first year)
Perfect use0.2%[36]
Typical use6%[36]
Usage
Duration effect3 months
(12–14 weeks)
Reversibility3–18 months
User remindersMaximum interval is just under 3 months
Clinic review12 weeks
Advantages and disadvantages
STI protectionNo
Period disadvantagesEspecially in first injection may be frequent spotting
Period advantagesUsually no periods from 2nd injection
BenefitsEspecially good if poor pill compliance.
Reduced endometrial cancer risk.
RisksReduced bone density, which may reverse after discontinuation
Medical notes
For those intending to start family, suggest switch 6 months prior to alternative method (e.g. POP) allowing more reliable return fertility.

DMPA, under brand names such as Depo-Provera and Depo-SubQ Provera 104, is used in hormonal birth control as a long-lasting progestogen-only injectable contraceptive to prevent pregnancy in women.[37][38] It is given by intramuscular or subcutaneous injection and forms a long-lasting depot, from which it is slowly released over a period of several months. It takes one week to take effect if given after the first five days of the period cycle, and is effective immediately if given during the first five days of the period cycle. Estimates of first-year failure rates are about 0.3%.[39]

Effectiveness

[edit]

Trussell's estimated perfect use first-year failure rate for DMPA as the average of failure rates in seven clinical trials at 0.3%.[39][40] It was considered perfect use because the clinical trials measured efficacy during actual use of DMPA defined as being no longer than 14 or 15 weeks after an injection (i.e., no more than 1 or 2 weeks late for a next injection).

Prior to 2004, Trussell's typical use failure rate for DMPA was the same as his perfect use failure rate: 0.3%.[41]

  • DMPA estimated typical use first-year failure rate = 0.3% in:
    • Contraceptive Technology, 16th revised edition (1994)[42]
    • Contraceptive Technology, 17th revised edition (1998)[43]
      • Adopted in 1998 by the FDA for its current Uniform Contraceptive Labeling guidance[44]

In 2004, using the 1995 NSFG failure rate, Trussell increased (by 10 times) his typical use failure rate for DMPA from 0.3% to 3%.[39][40]

  • DMPA estimated typical use first-year failure rate = 3% in:
    • Contraceptive Technology, 18th revised edition (2004)[39]
    • Contraceptive Technology, 19th revised edition (2007)[45]

Trussell did not use 1995 NSFG failure rates as typical use failure rates for the other two then newly available long-acting contraceptives, the Norplant implant (2.3%) and the ParaGard copper T 380A IUD (3.7%), which were (as with DMPA) an order of magnitude higher than in clinical trials. Since Norplant and ParaGard allow no scope for user error, their much higher 1995 NSFG failure rates were attributed by Trussell to contraceptive overreporting at the time of a conception leading to a live birth.[39][46][40]

Advantages

[edit]

DMPA has a number of advantages and benefits:[47][48][38][49]

The United Kingdom Department of Health has actively promoted Long Acting Reversible Contraceptive use since 2008, particularly for young people;[57] following on from the October 2005 National Institute for Health and Clinical Excellence guidelines.[58] Giving advice on these methods of contraception has been included in the 2009 Quality and Outcomes Framework "good practice" for primary care.[59]

Comparison

[edit]

Proponents of bioidentical hormone therapy believe that progesterone offers fewer side effects and improved quality of life compared to MPA.[60] The evidence for this view has been questioned; MPA is better absorbed when taken by mouth, with a much longer elimination half-life leading to more stable blood levels[61] though it may lead to greater breast tenderness and more sporadic vaginal bleeding.[60] The two compounds do not differentiate in their ability to suppress endometrial hyperplasia,[60] nor does either increase the risk of pulmonary embolism.[62] The two medications have not been adequately compared in direct tests to clear conclusions about safety and superiority.[24]

Available forms

[edit]
See also: Conjugated estrogens/medroxyprogesterone acetate, Estradiol/medroxyprogesterone acetate, and Estradiol cypionate/medroxyprogesterone acetate

MPA is available alone in the form of 2.5, 5, and 10 mg oral tablets, as a 150 mg/mL (1 mL) or 400 mg/mL (2.5 mL) microcrystalline aqueous suspension for intramuscular injection, and as a 104 mg (0.65 mL of 160 mg/mL) microcrystalline aqueous suspension for subcutaneous injection.[63][64] It has also been marketed in the form of 100, 200, 250, 400, and 500 mg oral tablets; 500 and 1,000 mg oral suspensions; and as a 50 mg/mL microcrystalline aqueous suspension for intramuscular injection.[65][66] A 100 mg/mL microcrystalline aqueous suspension for intramuscular injection was previously available as well.[63] In addition to single-drug formulations, MPA is available in the form of oral tablets in combination with conjugated estrogens (CEEs), estradiol, and estradiol valerate for use in menopausal hormone therapy, and is available in combination with estradiol cypionate in a microcrystalline aqueous suspension as a combined injectable contraceptive.[10][11][63][18]

Depo-Provera is the brand name for a 150 mg microcrystalline aqueous suspension of DMPA that is administered by intramuscular injection. The shot must be injected into thigh, buttock, or deltoid muscle four times a year (every 11 to 13 weeks), and provides pregnancy protection instantaneously after the first injection.[67] Depo-subQ Provera 104 is a variation of the original intramuscular DMPA that is instead a 104 mg microcrystalline dose in aqueous suspension administered by subcutaneous injection. It contains 69% of the MPA found in the original intramuscular DMPA formulation. It can be injected using a smaller injection needle inserting the medication just below the skin, instead of into the muscle, in either the abdomen or thigh. This subcutaneous injection claims to reduce the side effects of DMPA while still maintaining all the same benefits of the original intramuscular DMPA.

Contraindications

[edit]

MPA is not usually recommended because of unacceptable health risk or because it is not indicated in the following cases:[68][69]

Conditions where the theoretical or proven risks usually outweigh the advantages of using DMPA:

Conditions which represent an unacceptable health risk if DMPA is used:

Conditions where use is not indicated and should not be initiated:

MPA is not recommended for use prior to menarche or before or during recovery from surgery.[70]

Side effects

[edit]

In women, the most common adverse effects of MPA are acne, changes in menstrual flow, drowsiness, and can cause birth defects if taken by pregnant women. Other common side effects include breast tenderness, increased facial hair, decreased scalp hair, difficulty falling or remaining asleep, stomach pain, and weight loss or gain.[23] Lowered libido has been reported as a side effect of MPA in women.[71] DMPA can affect menstrual bleeding. After a year of use, 55% of women experience amenorrhea (missed periods); after two years, the rate rises to 68%. In the first months of use "irregular or unpredictable bleeding or spotting, or, rarely, heavy or continuous bleeding" was reported.[72] MPA does not appear to be associated with vitamin B12 deficiency.[73] Data on weight gain with DMPA likewise are inconsistent.[74][75]

At high doses for the treatment of breast cancer, MPA can cause weight gain and can worsen diabetes mellitus and edema (particularly of the face). Adverse effects peak at five weeks, and are reduced with lower doses. Less frequent effects may include thrombosis (though it is not clear if this is truly a risk, it cannot be ruled out), painful urination, headache, nausea, and vomiting. When used as a form of androgen deprivation therapy in men, more frequent complaints include reduced libido, impotence, reduced ejaculate volume, and within three days, chemical castration. At extremely high doses (used to treat cancer, not for contraception) MPA may cause adrenal suppression and may interfere with carbohydrate metabolism, but does not cause diabetes.[28]

When used as a form of injected birth control, there is a delayed return of fertility. The average return to fertility is 9 to 10 months after the last injection, taking longer for overweight or obese women. By 18 months after the last injection, fertility is the same as that in former users of other contraceptive methods.[47][48] Fetuses exposed to progestogens have demonstrated higher rates of genital abnormalities, low birth weight, and increased ectopic pregnancy particularly when MPA is used as an injected form of long-term birth control. A study of accidental pregnancies among poor women in Thailand found that infants who had been exposed to DMPA during pregnancy had a higher risk of low birth weight and an 80% greater-than-usual chance of dying in the first year of life.[76] There were noticeable adverse effects to the cardiovascular system of those who took the treatment.[77] It was also found that after the user had stopped taking the treatment, bone density changes were observed [78] The formation of meningiomas due to the treatment have been the subject of lawsuits.[79] Blood pressure changes were observed in addition to bone density changes.[80]

Mood changes

[edit]

There have been concerns about a possible risk of depression and mood changes with progestins like MPA, and this has led to reluctance of some clinicians and women to use them.[81][82] However, contrary to widely held beliefs, most research suggests that progestins do not cause adverse psychological effects such as depression or anxiety.[81] A 2018 systematic review of the relationship between progestin-based contraception and depression included three large studies of DMPA and reported no association between DMPA and depression.[83] According to a 2003 review of DMPA, the majority of published clinical studies indicate that DMPA is not associated with depression, and the overall data support the notion that the medication does not significantly affect mood.[84]

In the largest study to have assessed the relationship between MPA and depression to date, in which over 3,900 women were treated with DMPA for up to 7 years, the incidence of depression was infrequent at 1.5% and the discontinuation rate due to depression was 0.5%.[83][37][85] This study did not include baseline data on depression,[85] and due to the incidence of depression in the study, the FDA required package labeling for DMPA stating that women with depression should be observed carefully and that DMPA should be discontinued if depression recurs.[83] A subsequent study of 495 women treated with DMPA over the course of 1 year found that the mean depression score slightly decreased in the whole group of continuing users from 7.4 to 6.7 (by 9.5%) and decreased in the quintile of that group with the highest depression scores at baseline from 15.4 to 9.5 (by 38%).[85] Based on the results of this study and others, a consensus began emerging that DMPA does not in fact increase the risk of depression nor worsen the severity of pre-existing depression.[75][85][37]

Similarly to the case of DMPA for hormonal contraception, the Heart and Estrogen/Progestin Replacement Study (HERS), a study of 2,763 postmenopausal women treated with 0.625 mg/day oral CEEs plus 2.5 mg/day oral MPA or placebo for 36 months as a method of menopausal hormone therapy, found no change in depressive symptoms.[86][87][88] However, some small studies have reported that progestins like MPA might counteract beneficial effects of estrogens against depression.[81][3][89]

Long-term effects

[edit]

The Women's Health Initiative investigated the use of a combination of oral CEEs and MPA compared to placebo. The study was prematurely terminated when previously unexpected risks were discovered, specifically the finding that though the all-cause mortality was not affected by the hormone therapy, the benefits of menopausal hormone therapy (reduced risk of hip fracture, colorectal and endometrial cancer and all other causes of death) were offset by increased risk of coronary heart disease, breast cancer, strokes and pulmonary embolism.[90]

When combined with CEEs, MPA has been associated with an increased risk of breast cancer, dementia, and thrombus in the eye. In combination with estrogens in general, MPA may increase the risk of cardiovascular disease, with a stronger association when used by postmenopausal women also taking CEEs. It was because of these unexpected interactions that the Women's Health Initiative study was ended early due to the extra risks of menopausal hormone therapy,[91] resulting in a dramatic decrease in both new and renewal prescriptions for hormone therapy.[92]

Long-term studies of users of DMPA have found slight or no increased overall risk of breast cancer. However, the study population did show a slightly increased risk of breast cancer in recent users (DMPA use in the last four years) under age 35, similar to that seen with the use of combined oral contraceptive pills.[72]

Results of the Women's Health Initiative (WHI) menopausal hormone therapy randomized controlled trials
Clinical outcome Hypothesized
effect on risk 		Estrogen and progestogen
(CEsTooltip conjugated estrogens 0.625 mg/day p.o. + MPATooltip medroxyprogesterone acetate 2.5 mg/day p.o.)
(n = 16,608, with uterus, 5.2–5.6 years follow up) 		Estrogen alone
(CEsTooltip Conjugated estrogens 0.625 mg/day p.o.)
(n = 10,739, no uterus, 6.8–7.1 years follow up)
HRTooltip Hazard ratio 95% CITooltip Confidence interval ARTooltip Attributable risk HRTooltip Hazard ratio 95% CITooltip Confidence interval ARTooltip Attributable risk
Coronary heart disease Decreased 1.24 1.00–1.54 +6 / 10,000 PYs 0.95 0.79–1.15 −3 / 10,000 PYs
Stroke Decreased 1.31 1.02–1.68 +8 / 10,000 PYs 1.37 1.09–1.73 +12 / 10,000 PYs
Pulmonary embolism Increased 2.13 1.45–3.11 +10 / 10,000 PYs 1.37 0.90–2.07 +4 / 10,000 PYs
Venous thromboembolism Increased 2.06 1.57–2.70 +18 / 10,000 PYs 1.32 0.99–1.75 +8 / 10,000 PYs
Breast cancer Increased 1.24 1.02–1.50 +8 / 10,000 PYs 0.80 0.62–1.04 −6 / 10,000 PYs
Colorectal cancer Decreased 0.56 0.38–0.81 −7 / 10,000 PYs 1.08 0.75–1.55 +1 / 10,000 PYs
Endometrial cancer 0.81 0.48–1.36 −1 / 10,000 PYs
Hip fractures Decreased 0.67 0.47–0.96 −5 / 10,000 PYs 0.65 0.45–0.94 −7 / 10,000 PYs
Total fractures Decreased 0.76 0.69–0.83 −47 / 10,000 PYs 0.71 0.64–0.80 −53 / 10,000 PYs
Total mortality Decreased 0.98 0.82–1.18 −1 / 10,000 PYs 1.04 0.91–1.12 +3 / 10,000 PYs
Global index 1.15 1.03–1.28 +19 / 10,000 PYs 1.01 1.09–1.12 +2 / 10,000 PYs
Diabetes 0.79 0.67–0.93 0.88 0.77–1.01
Gallbladder disease Increased 1.59 1.28–1.97 1.67 1.35–2.06
Stress incontinence 1.87 1.61–2.18 2.15 1.77–2.82
Urge incontinence 1.15 0.99–1.34 1.32 1.10–1.58
Peripheral artery disease 0.89 0.63–1.25 1.32 0.99–1.77
Probable dementia Decreased 2.05 1.21–3.48 1.49 0.83–2.66
Abbreviations: CEs = conjugated estrogens. MPA = medroxyprogesterone acetate. p.o. = per oral. HR = hazard ratio. AR = attributable risk. PYs = person–years. CI = confidence interval. Notes: Sample sizes (n) include placebo recipients, which were about half of patients. "Global index" is defined for each woman as the time to earliest diagnosis for coronary heart disease, stroke, pulmonary embolism, breast cancer, colorectal cancer, endometrial cancer (estrogen plus progestogen group only), hip fractures, and death from other causes. Sources: See template.

Blood clots

[edit]

DMPA has been associated in multiple studies with a higher risk of venous thromboembolism (VTE) when used as a form of progestogen-only birth control in premenopausal women.[93][94][95][96] The increase in incidence of VTE ranges from 2.2-fold to 3.6-fold.[93][94][95][96] Elevated risk of VTE with DMPA is unexpected, as DMPA has little or no effect on coagulation and fibrinolytic factors,[97][98] and progestogens by themselves normally do not increase the risk of thrombosis.[94][95] It has been argued that the higher incidence with DMPA has reflected preferential prescription of DMPA to women considered to be at an increased risk of VTE.[94] Alternatively, it is possible that MPA may be an exception among progestins in terms of VTE risk.[99][100][101] A 2018 meta-analysis reported that MPA was associated with a 2.8-fold higher risk of VTE than other progestins.[100] It is possible that the glucocorticoid activity of MPA may increase the risk of VTE.[3][102][101]

Bone density

[edit]

DMPA may cause reduced bone density in premenopausal women and in men when used without an estrogen, particularly at high doses, though this appears to be reversible to a normal level even after years of use.

On 17 November 2004, the United States Food and Drug Administration put a black box warning on the label, indicating that there were potential adverse effects of loss of bone mineral density.[103][104] While it causes temporary bone loss, most women fully regain their bone density after discontinuing use.[74] The World Health Organization (WHO) recommends that the use not be restricted.[105][106] The American College of Obstetricians and Gynecologists notes that the potential adverse effects on BMD be balanced against the known negative effects of unintended pregnancy using other birth control methods or no method, particularly among adolescents.

Three studies have suggested that bone loss is reversible after the discontinuation of DMPA.[107][108][109] Other studies have suggested that the effect of DMPA use on postmenopausal bone density is minimal,[110] perhaps because DMPA users experience less bone loss at menopause.[111] Use after peak bone mass is associated with increased bone turnover but no decrease in bone mineral density.[112]

The FDA recommends that DMPA not be used for longer than two years, unless there is no viable alternative method of contraception, due to concerns over bone loss.[104] However, a 2008 Committee Opinion from the American Congress of Obstetricians and Gynecologists (ACOG) advises healthcare providers that concerns about bone mineral density loss should neither prevent the prescription of or continuation of DMPA beyond two years of use.[113]

HIV risk

[edit]

There is uncertainty regarding the risk of HIV acquisition among DMPA users; some observational studies suggest an increased risk of HIV acquisition among women using DMPA, while others do not.[114] The World Health Organization issued statements in February 2012 and July 2014 saying the data did not warrant changing their recommendation of no restriction – Medical Eligibility for Contraception (MEC) category 1 – on the use of DMPA in women at high risk for HIV.[115][116] Two meta-analyses of observational studies in sub-Saharan Africa were published in January 2015.[117] They found a 1.4- to 1.5-fold increase risk of HIV acquisition for DMPA users relative to no hormonal contraceptive use.[118][119] In January 2015, the Faculty of Sexual & Reproductive Healthcare of the Royal College of Obstetricians and Gynaecologists issued a statement reaffirming that there is no reason to advise against use of DMPA in the United Kingdom even for women at 'high risk' of HIV infection.[120] A systematic review and meta-analysis of risk of HIV infection in DMPA users published in fall of 2015 stated that "the epidemiological and biological evidence now make a compelling case that DMPA adds significantly to the risk of male-to-female HIV transmission."[121] In 2019, a randomized controlled trial found no significant association between DMPA use and HIV.[122]

Breastfeeding

[edit]

MPA may be used by breastfeeding mothers. Heavy bleeding is possible if given in the immediate postpartum time and is best delayed until six weeks after birth. It may be used within five days if not breast feeding. While a study showed "no significant difference in birth weights or incidence of birth defects" and "no significant alternation of immunity to infectious disease caused by breast milk containing DMPA", a subgroup of babies whose mothers started DMPA at two days postpartum had a 75% higher incidence of doctor visits for infectious diseases during their first year of life.[123]

A larger study with longer follow-up concluded that "use of DMPA during pregnancy or breastfeeding does not adversely affect the long-term growth and development of children". This study also noted that "children with DMPA exposure during pregnancy and lactation had an increased risk of suboptimal growth in height," but that "after adjustment for socioeconomic factors by multiple logistic regression, there was no increased risk of impaired growth among the DMPA-exposed children." The study also noted that effects of DMPA exposure on puberty require further study, as so few children over the age of 10 were observed.[124]

Overdose

[edit]

MPA has been studied at "massive" dosages of up to 5,000 mg per day orally and 2,000 mg per day via intramuscular injection, without major tolerability or safety issues described.[125][126][127] Overdose is not described in the Food and Drug Administration (FDA) product labels for injected MPA (Depo-Provera or Depo-SubQ Provera 104).[6][7] In the FDA product label for oral MPA (Provera), it is stated that overdose of an estrogen and progestin may cause nausea and vomiting, breast tenderness, dizziness, abdominal pain, drowsiness, fatigue, and withdrawal bleeding.[5] According to the label, treatment of overdose should consist of discontinuation of MPA therapy and symptomatic care.[5]

Interactions

[edit]

MPA increases the risk of breast cancer, dementia, and thrombus when used in combination with CEEs to treat menopausal symptoms.[70] When used as a contraceptive, MPA does not generally interact with other medications. The combination of MPA with aminoglutethimide to treat metastases from breast cancer has been associated with an increase in depression.[28] St John's wort may decrease the effectiveness of MPA as a contraceptive due to acceleration of its metabolism.[70]

Pharmacology

[edit]

Pharmacodynamics

[edit]

MPA acts as an agonist of the progesterone, androgen, and glucocorticoid receptors (PR, AR, and GR, respectively),[4] activating these receptors with EC50 values of approximately 0.01 nM, 1 nM, and 10 nM, respectively.[128] It has negligible affinity for the estrogen receptor.[4] The medication has relatively high affinity for the mineralocorticoid receptor, but in spite of this, it has no mineralocorticoid or antimineralocorticoid activity.[3] The intrinsic activities of MPA in activating the PR and the AR have been reported to be at least equivalent to those of progesterone and dihydrotestosterone (DHT), respectively, indicating that it is a full agonist of these receptors.[129][130]

Relative affinities (%) of MPA and related steroids
Progestogen
 PRTooltip Progesterone receptor ARTooltip Androgen receptor ERTooltip Estrogen receptor GRTooltip Glucocorticoid receptor MRTooltip Mineralocorticoid receptor
Progesterone 50 0 0 10 100
Chlormadinone acetate 67 5 0 8 0
Cyproterone acetate 90 6 0 6 8
Medroxyprogesterone acetate 115 5 0 29 160
Megestrol acetate 65 5 0 30 0
Notes: Values are percentages (%). Reference ligands (100%) were promegestone for the PRTooltip progesterone receptor, metribolone for the ARTooltip androgen receptor, estradiol for the ERTooltip estrogen receptor, dexamethasone for the GRTooltip glucocorticoid receptor, and aldosterone for the MRTooltip mineralocorticoid receptor. Sources:[3]

Progestogenic activity

[edit]

MPA is a potent agonist of the progesterone receptor with similar affinity and efficacy relative to progesterone.[131] While both MPA and its deacetylated analogue medroxyprogesterone bind to and agonize the PR, MPA has approximately 100-fold higher binding affinity and transactivation potency in comparison.[131] As such, unlike MPA, medroxyprogesterone is not used clinically, though it has seen some use in veterinary medicine.[132] The oral dosage of MPA required to inhibit ovulation (i.e., the effective contraceptive dosage) is 10 mg/day, whereas 5 mg/day was not sufficient to inhibit ovulation in all women.[133] In accordance, the dosage of MPA used in oral contraceptives in the past was 10 mg per tablet.[134] For comparison to MPA, the dosage of progesterone required to inhibit ovulation is 300 mg/day, whereas that of the 19-nortestosterone derivatives norethisterone and norethisterone acetate is only 0.4 to 0.5 mg/day.[135]

The mechanism of action of progestogen-only contraceptives like DMPA depends on the progestogen activity and dose. High-dose progestogen-only contraceptives, such as DMPA, inhibit follicular development and prevent ovulation as their primary mechanism of action.[136][137] The progestogen decreases the pulse frequency of gonadotropin-releasing hormone (GnRH) release by the hypothalamus, which decreases the release of follicle-stimulating hormone (FSH) and luteinizing hormone (LH) by the anterior pituitary. Decreased levels of FSH inhibit follicular development, preventing an increase in estradiol levels. Progestogen negative feedback and the lack of estrogen positive feedback on LH release prevent a LH surge. Inhibition of follicular development and the absence of a LH surge prevent ovulation.[47][48] A secondary mechanism of action of all progestogen-containing contraceptives is inhibition of sperm penetration by changes in the cervical mucus.[138] Inhibition of ovarian function during DMPA use causes the endometrium to become thin and atrophic. These changes in the endometrium could, theoretically, prevent implantation. However, because DMPA is highly effective in inhibiting ovulation and sperm penetration, the possibility of fertilization is negligible. No available data support prevention of implantation as a mechanism of action of DMPA.[138]

MPA and related steroids at the progesterone receptor
Compound Ki (nM) EC50Tooltip Half-maximal effective concentration (nM)a EC50Tooltip Half-maximal effective concentration (nM)b
Progesterone 4.3 0.9 25
Medroxyprogesterone 241 47 32
Medroxyprogesterone acetate 1.2 0.6 0.15
Footnotes: a = Coactivator recruitment. b = Reporter cell line. Sources:[131]
Oral potencies of MPA and related steroids
Progestogen OID
(mg/day)		 TFD
(mg/cycle)		 TFD
(mg/day)		 ODP
(mg/day)		 ECD
(mg/day)
Progesterone 300 4200 200–300 200
Chlormadinone acetate 1.7 20–30 10 2.0 5–10
Cyproterone acetate 1.0 20 1.0 2.0 1.0
Medroxyprogesterone acetate 10 50 5–10 ? 5.0
Megestrol acetate ? 50 ? ? 5.0
Abbreviations: OID = ovulation-inhibiting dosage (without additional estrogen). TFD = endometrial transformation dosage. ODP = oral dosage in commercial contraceptive preparations. ECD = estimated comparable dosage. Sources:[135][102][139]
Parenteral potencies and durations of progestogens[a][b]
Compound Form Dose for specific uses (mg)[c] DOA[d]
TFD[e] POICD[f] CICD[g]
Algestone acetophenide Oil soln. 75–150 14–32 d
Gestonorone caproate Oil soln. 25–50 8–13 d
Hydroxyprogest. acetate[h] Aq. susp. 350 9–16 d
Hydroxyprogest. caproate Oil soln. 250–500[i] 250–500 5–21 d
Medroxyprog. acetate Aq. susp. 50–100 150 25 14–50+ d
Megestrol acetate Aq. susp. 25 >14 d
Norethisterone enanthate Oil soln. 100–200 200 50 11–52 d
Progesterone Oil soln. 200[i] 2–6 d
Aq. soln. ? 1–2 d
Aq. susp. 50–200 7–14 d
Notes and sources:
  1. ^ Sources: [140][141][142][143][144][145][146][147][148][149][150][151][152][153][154][155][156][157][158]
  2. ^ All given by intramuscular or subcutaneous injection.
  3. ^ Progesterone production during the luteal phase is ~25 (15–50) mg/day. The OIDTooltip ovulation-inhibiting dose of OHPC is 250 to 500 mg/month.
  4. ^ Duration of action in days.
  5. ^ Usually given for 14 days.
  6. ^ Usually dosed every two to three months.
  7. ^ Usually dosed once monthly.
  8. ^ Never marketed or approved by this route.
  9. ^ a b In divided doses (2 × 125 or 250 mg for OHPC, 10 × 20 mg for P4).

Antigonadotropic and anticorticotropic effects

[edit]

MPA suppresses the hypothalamic–pituitary–adrenal (HPA) and hypothalamic–pituitary–gonadal (HPG) axes at sufficient dosages, resulting decreased levels of gonadotropins, androgens, estrogens, adrenocorticotropic hormone (ACTH), and cortisol, as well as levels of sex hormone-binding globulin (SHBG).[12] There is evidence that the suppressive effects of MPA on the HPG axis are mediated by activation of both the PR and the AR in the pituitary gland.[159][160] Due to its effects on androgen levels, MPA can produce strong functional antiandrogenic effects, and is used in the treatment of androgen-dependent conditions such as precocious puberty in boys and hypersexuality in men.[161] In addition, since the medication suppresses estrogen levels as well, MPA can produce strong functional antiestrogenic effects similarly, and has been used to treat estrogen-dependent conditions such as precocious puberty in girls and endometriosis in women. Due to low estrogen levels, the use of MPA without an estrogen poses a risk of decreased bone mineral density and other symptoms of estrogen deficiency.[162]

Oral MPA has been found to suppress testosterone levels in men by about 30% (from 831 ng/dL to 585 ng/dL) at a dosage of 20 mg/day, by about 45–75% (average 60%; to 150–400 ng/dL) at a dosage of 60 mg/day,[163][164][165] and by about 70–75% (from 832 to 862 ng/dL to 214 to 251 ng/dL) at a dosage of 100 mg/day.[166][167] Dosages of oral MPA of 2.5 to 30 mg/day in combination with estrogens have been used to help suppress testosterone levels in transgender women.[168][169][170][171][172][173] One study of injectable MPA in men with benign prostatic hyperplasia reported that a single 150 mg dose suppressed testosterone levels into the defined male castrate range (<58 ng/dL) within 7 days and that castration levels of testosterone were maintained for 3 months.[174] Very high doses of intramuscular MPA of 150 to 500 mg per week (but up to 900 mg per week) have similarly been reported to suppress testosterone levels to less than 100 ng/dL.[163][175] The typical initial dose of intramuscular MPA for testosterone suppression in men with paraphilias is 400 or 500 mg per week.[163]

Androgenic activity

[edit]

MPA is a potent full agonist of the AR. Its activation of the AR may play an important and major role in its antigonadotropic effects and in its beneficial effects against breast cancer.[159][176][177] However, although MPA may produce androgenic side effects such as acne and hirsutism in some women,.[178][179] In fact, likely due to its suppressive actions on androgen levels, it has been reported that MPA is generally highly effective in improving pre-existing symptoms of hirsutism in women with the condition.[180][181] However, MPA has been seen to cause androgenic effects in children with precocious puberty.[182] The reason for the general lack of virilizing effects with MPA, despite it binding to and activating the AR with high affinity and this action potentially playing an important role in many of its physiological and therapeutic effects, is not entirely clear. However, MPA has been found to interact with the AR differently compared to other agonists of the receptor such as dihydrotestosterone (DHT).[129] The result of this difference appears to be that MPA binds to the AR with a similar affinity and intrinsic activity to that of DHT, but requires about 100-fold higher concentrations for a comparable induction of gene transcription, while at the same time not antagonizing the transcriptional activity of normal androgens like DHT at any concentration.[129] Thus, this may explain the low propensity of MPA for producing androgenic side effects.[129]

MPA shows weak androgenic effects on liver protein synthesis, similarly to other weakly androgenic progestins like megestrol acetate and 19-nortestosterone derivatives.[3][8] While it does not antagonize estrogen-induced increases in levels of triglycerides and HDL cholesterol, DMPA every other week may decrease levels of HDL cholesterol.[3] In addition, MPA has been found to suppress sex hormone-binding globulin (SHBG) production by the liver.[8][183][184] At a dosage of 10 mg/day oral MPA, it has been found to decrease circulating SHBG levels by 14–18% in women taking 4 mg/day oral estradiol valerate.[8] Conversely, in a study that combined 2.5 mg/day oral MPA with various oral estrogens, no influence of MPA on estrogen-induced increases in SHBG levels was discerned.[184] In another, higher-dose study, SHBG levels were lower by 59% in a group of women treated with 50 mg/day oral MPA alone relative to an untreated control group of women.[183] In massive-dose studies of oral or injectable MPA (e.g., 500–1,000 mg/day), the medication decreased SHBG levels by about 80%.[185][186][187]

Unlike the related steroids megestrol acetate and cyproterone acetate, MPA is not an antagonist of the AR and does not have direct antiandrogenic activity.[3] As such, although MPA is sometimes described as an antiandrogen, it is not a "true" antiandrogen (i.e., AR antagonist).[164]

Glucocorticoid activity

[edit]

As an agonist of the GR, MPA has glucocorticoid activity, and as a result can cause symptoms of Cushing's syndrome,[188] steroid diabetes, and adrenal insufficiency at sufficiently high doses.[189] It has been suggested that the glucocorticoid activity of MPA may contribute to bone loss.[190] The glucocorticoid activity of MPA may also result in an upregulation of the thrombin receptor in blood vessel walls, which may contribute to procoagulant effects of MPA and risk of venous thromboembolism and atherosclerosis.[3] The relative glucocorticoid activity of MPA is among the highest of the clinically used progestins.[3]

Glucocorticoid activity of selected steroids in vitro
Steroid Class TRTooltip Thrombin receptor ()a GRTooltip glucocorticoid receptor (%)b
Dexamethasone Corticosteroid ++ 100
Ethinylestradiol Estrogen 0
Etonogestrel Progestin + 14
Gestodene Progestin + 27
Levonorgestrel Progestin 1
Medroxyprogesterone acetate Progestin + 29
Norethisterone Progestin 0
Norgestimate Progestin 1
Progesterone Progestogen + 10
Footnotes: a = Thrombin receptor (TR) upregulation (↑) in vascular smooth muscle cells (VSMCs). b = RBATooltip Relative binding affinity (%) for the glucocorticoid receptor (GR). Strength: – = No effect. + = Pronounced effect. ++ = Strong effect. Sources: [191]

Steroidogenesis inhibition

[edit]
See also: Steroidogenesis inhibitor and Neurosteroidogenesis inhibitor

MPA has been found to act as a competitive inhibitor of rat 3α-hydroxysteroid dehydrogenase (3α-HSD).[192][193][194][195] This enzyme is essential for the transformation of progesterone, deoxycorticosterone, and DHT into inhibitory neurosteroids such as allopregnanolone, THDOCTooltip tetrahydrodeoxycorticosterone, and 3α-androstanediol, respectively.[196] MPA has been described as very potent in its inhibition of rat 3α-HSD, with an IC50 of 0.2 μM and a Ki (in rat testicular homogenates) of 0.42 μM.[192][193] However, inhibition of 3α-HSD by MPA does not appear to have been confirmed using human proteins yet, and the concentrations required with rat proteins are far above typical human therapeutic concentrations.[192][193]

MPA has been identified as a competitive inhibitor of human 3β-hydroxysteroid dehydrogenase/Δ5-4 isomerase II (3β-HSD II).[197] This enzyme is essential for the biosynthesis of sex steroids and corticosteroids.[197] The Ki of MPA for inhibition of 3β-HSD II is 3.0 μM, and this concentration is reportedly near the circulating levels of the medication that are achieved by very high therapeutic dosages of MPA of 5 to 20 mg/kg/day (dosages of 300 to 1,200 mg/day for a 60 kg (132 lb) person).[197] Aside from 3β-HSD II, other human steroidogenic enzymes, including cholesterol side-chain cleavage enzyme (P450scc/CYP11A1) and 17α-hydroxylase/17,20-lyase (CYP17A1), were not found to be inhibited by MPA.[197] MPA has been found to be effective in the treatment of gonadotropin-independent precocious puberty and in breast cancer in postmenopausal women at high dosages, and inhibition of 3β-HSD II could be responsible for its effectiveness in these conditions.[197]

GABAA receptor allosteric modulation

[edit]

Progesterone, via transformation into neurosteroids such as 5α-dihydroprogesterone, 5β-dihydroprogesterone, allopregnanolone, and pregnanolone (catalyzed by the enzymes 5α- and 5β-reductase and 3α- and 3β-HSD), is a positive allosteric modulator of the GABAA receptor, and is associated with a variety of effects mediated by this property including dizziness, sedation, hypnotic states, mood changes, anxiolysis, and cognitive/memory impairment, as well as effectiveness as an anticonvulsant in the treatment of catamenial epilepsy.[196][198] It has also been found to produce anesthesia via this action in animals when administered at sufficiently high dosages.[198] MPA was found to significantly reduce seizure incidence when added to existing anticonvulsant regimens in 11 of 14 women with uncontrolled epilepsy, and has also been reported to induce anesthesia in animals, raising the possibility that it might modulate the GABAA receptor similarly to progesterone.[199][200]

MPA shares some of the same metabolic routes of progesterone and, analogously, can be transformed into metabolites such as 5α-dihydro-MPA (DHMPA) and 3α,5α-tetrahydro-MPA (THMPA).[199] However, unlike the reduced metabolites of progesterone, DHMPA and THMPA have been found not to modulate the GABAA receptor.[199] Conversely, unlike progesterone, MPA itself actually modulates the GABAA receptor, although notably not at the neurosteroid binding site.[199] However, rather than act as a potentiator of the receptor, MPA appears to act as a negative allosteric modulator.[199] Whereas the reduced metabolites of progesterone enhance binding of the benzodiazepine flunitrazepam to the GABAA receptor in vitro, MPA can partially inhibit the binding of flunitrazepam by up to 40% with half-maximal inhibition at 1 μM.[199] However, the concentrations of MPA required for inhibition are high relative to therapeutic concentrations, and hence, this action is probably of little or no clinical relevance.[199] The lack of potentiation of the GABAA receptor by MPA or its metabolites is surprising in consideration of the apparent anticonvulsant and anesthetic effects of MPA described above, and they remain unexplained.[199]

Clinical studies using massive dosages of up to 5,000 mg/day oral MPA and 2,000 mg/day intramuscular MPA for 30 days in women with advanced breast cancer have reported "no relevant side effects", which suggests that MPA has no meaningful direct action on the GABAA receptor in humans even at extremely high dosages.[125]

Appetite stimulation

[edit]

Although MPA and the closely related medication megestrol acetate are effective appetite stimulants at very high dosages,[201] the mechanism of action of their beneficial effects on appetite is not entirely clear. However, glucocorticoid, cytokine, and possibly anabolic-related mechanisms are all thought to possibly be involved, and a number of downstream changes have been implicated, including stimulation of the release of neuropeptide Y in the hypothalamus, modulation of calcium channels in the ventromedial hypothalamus, and inhibition of the secretion of proinflammatory cytokines including IL-1α, IL-1β, IL-6, and TNF-α, actions that have all been linked to an increase in appetite.[202]

Other activity

[edit]

MPA weakly stimulates the proliferation of MCF-7 breast cancer cells in vitro, an action that is independent of the classical PRs and is instead mediated via the progesterone receptor membrane component-1 (PGRMC1).[203] Certain other progestins are also active in this assay, whereas progesterone acts neutrally.[203] It is unclear if these findings may explain the different risks of breast cancer observed with progesterone, dydrogesterone, and other progestins such as medroxyprogesterone acetate and norethisterone in clinical studies.[204]

Pharmacokinetics

[edit]

Absorption

[edit]

Surprisingly few studies have been conducted on the pharmacokinetics of MPA at postmenopausal replacement dosages.[205][3] The bioavailability of MPA with oral administration is approximately 100%.[3] A single oral dose of 10 mg MPA has been found to result in peak MPA levels of 1.2 to 5.2 ng/mL within 2 hours of administration using radioimmunoassay.[205][206] Following this, levels of MPA decreased to 0.09 to 0.35 ng/mL 12 hours post-administration.[205][206] In another study, peak levels of MPA were 3.4 to 4.4 ng/mL within 1 to 4 hours of administration of 10 mg oral MPA using radioimmunoassay.[205][207] Subsequently, MPA levels fell to 0.3 to 0.6 ng/mL 24 hours after administration.[205][207] In a third study, MPA levels were 4.2 to 4.4 ng/mL after an oral dose of 5 mg MPA and 6.0 ng/mL after an oral dose of 10 mg MPA, both using radioimmunoassay as well.[205][208]

Treatment of postmenopausal women with 2.5 or 5 mg/day MPA in combination with estradiol valerate for two weeks has been found to rapidly increase circulating MPA levels, with steady-state concentrations achieved after three days and peak concentrations occurring 1.5 to 2 hours after ingestion.[3][209] With 2.5 mg/day MPA, levels of the medication were 0.3 ng/mL (0.8 nmol/L) in women under 60 years of age and 0.45 ng/mL (1.2 nmol/L) in women 65 years of age or over, and with 5 mg/day MPA, levels were 0.6 ng/mL (1.6 nmol/L) in women under 60 years of age and in women 65 years of age or over.[3][209] Hence, area-under-curve levels of the medication were 1.6 to 1.8 times higher in those who were 65 years of age or older relative to those who were 60 years of age or younger.[8][209] As such, levels of MPA have been found to vary with age, and MPA may have an increased risk of side effects in elderly postmenopausal women.[8][3][209] This study assessed MPA levels using liquid-chromatography–tandem mass spectrometry (LC–MS/MS), a more accurate method of blood determinations.[209]

Oral MPA tablets can be administered sublingually instead of orally.[210][211][212] Rectal administration of MPA has also been studied.[213]

With intramuscular administration of 150 mg microcrystalline MPA in aqueous suspension, the medication is detectable in the circulation within 30 minutes, serum concentrations vary but generally plateau at 1.0 ng/mL (2.6 nmol/L) for 3 months.[214] Following this, there is a gradual decline in MPA levels, and the medication can be detected in the circulation for as long as 6 to 9 months post-injection.[214] The particle size of MPA crystals significantly influences its rate of absorption into the body from the local tissue depot when used as a microcrystalline aqueous suspension via intramuscular injection.[215][216][217] Smaller crystals dissolve faster and are absorbed more rapidly, resulting in a shorter duration of action.[215][216][217] Particle sizes can differ between different formulations of MPA, potentially influencing clinical efficacy and tolerability.[215][216][217][218]

Distribution

[edit]

The plasma protein binding of MPA is 88%.[3][8] It is weakly bound to albumin and is not bound to sex hormone-binding globulin or corticosteroid-binding globulin.[3][8]

Metabolism

[edit]

The elimination half-life of MPA via oral administration has been reported as both 11.6 to 16.6 hours[5] and 33 hours,[3] whereas the elimination half-lives with intramuscular and subcutaneous injection of microcrystalline MPA in aqueous suspension are 50 and 40 days, respectively.[6][7] The metabolism of MPA is mainly via hydroxylation, including at positions C6β, C21, C2β, and C1β, mediated primarily via CYP3A4, but 3- and 5-dihydro and 3,5-tetrahydro metabolites of MPA are also formed.[3][8] Deacetylation of MPA and its metabolites (into, e.g., medroxyprogesterone) has been observed to occur in non-human primate research to a substantial extent as well (30 to 70%).[219] MPA and/or its metabolites are also metabolized via conjugation.[70] The C6α methyl and C17α acetoxy groups of MPA make it more resistant to metabolism and allow for greater bioavailability than oral progesterone.[8]

Elimination

[edit]

MPA is eliminated 20 to 50% in urine and 5 to 10% in feces following intravenous administration.[220] Less than 3% of a dose is excreted in unconjugated form.[220]

Level–effect relationships

[edit]

With intramuscular administration, the high levels of MPA in the blood inhibit luteinizing hormone and ovulation for several months, with an accompanying decrease in serum progesterone to below 0.4 ng/mL.[214] Ovulation resumes when once blood levels of MPA fall below 0.1 ng/mL.[214] Serum estradiol remains at approximately 50 pg/mL for approximately four months post-injection (with a range of 10–92 pg/mL after several years of use), rising once MPA levels fall below 0.5 ng/mL.[214]

Hot flashes are rare while MPA is found at significant blood levels in the body, and the vaginal lining remains moist and creased. The endometrium undergoes atrophy, with small, straight glands and a stroma that is decidualized. Cervical mucus remains viscous. Because of its steady blood levels over the long term and multiple effects that prevent fertilization, MPA is a very effective means of birth control.[214]

Time–concentration curves

[edit]
Hormone levels with medroxyprogesterone acetate

Chemistry

[edit]
See also: List of progestogens, Progestogen ester, List of progestogen esters, Steroidal antiandrogen, and List of steroidal antiandrogens

MPA is a synthetic pregnane steroid and a derivative of progesterone and 17α-hydroxyprogesterone.[224][132] Specifically, it is the 17α-acetate ester of medroxyprogesterone or the 6α-methylated analogue of hydroxyprogesterone acetate.[224][132] MPA is known chemically as 6α-methyl-17α-acetoxyprogesterone or as 6α-methyl-17α-acetoxypregn-4-ene-3,20-dione, and its generic name is a contraction of 6α-methyl-17α-hydroxyprogesterone acetate.[224][132] MPA is closely related to other 17α-hydroxyprogesterone derivatives such as chlormadinone acetate, cyproterone acetate, and megestrol acetate, as well as to medrogestone and nomegestrol acetate.[224][132] 9α-fluoromedroxyprogesterone acetate (FMPA), the C9α fluoro analogue of MPA and an angiogenesis inhibitor with two orders of magnitude greater potency in comparison to MPA, was investigated for the potential treatment of cancers but was never marketed.[225][226]

History

[edit]

MPA was independently discovered in 1956 by Syntex and the Upjohn Company.[13][14][227][228] It was first introduced on 18 June 1959 by Upjohn in the United States under the brand name Provera (2.5, 5, and 10 mg tablets) for the treatment of amenorrhea, metrorrhagia, and recurrent miscarriage.[229][230] An intramuscular formulation of MPA, now known as DMPA (400 mg/mL MPA), was also introduced, under the brand name brand name Depo-Provera, in 1960 in the U.S. for the treatment of endometrial and renal cancer.[27] MPA in combination with ethinylestradiol was introduced in 1964 by Upjohn in the U.S. under the brand name Provest (10 mg MPA and 50 μg ethinylestradiol tablets) as an oral contraceptive, but this formulation was discontinued in 1970.[231][232][134] This formulation was marketed by Upjohn outside of the U.S. under the brand names Provestral and Provestrol, while Cyclo-Farlutal (or Ciclofarlutal) and Nogest-S[233] were formulations available outside of the U.S. with a different dosage (5 mg MPA and 50 or 75 μg ethinylestradiol tablets).[234][235]

Following its development in the late 1950s, DMPA was first assessed in clinical trials for use as an injectable contraceptive in 1963.[236] Upjohn sought FDATooltip Food and Drug Administration approval of intramuscular DMPA as a long-acting contraceptive under the brand name Depo-Provera (150 mg/mL MPA) in 1967, but the application was rejected.[237][238] However, this formulation was successfully introduced in countries outside of the United States for the first time in 1969, and was available in over 90 countries worldwide by 1992.[35] Upjohn attempted to gain FDA approval of DMPA as a contraceptive again in 1978, and yet again in 1983, but both applications failed similarly to the 1967 application.[237][238] However, in 1992, the medication was finally approved by the FDA, under the brand name Depo-Provera, for use in contraception.[237] A subcutaneous formulation of DMPA was introduced in the United States as a contraceptive under the brand name Depo-SubQ Provera 104 (104 mg/0.65 mL MPA) in December 2004, and subsequently was also approved for the treatment of endometriosis-related pelvic pain.[239]

MPA has also been marketed widely throughout the world under numerous other brand names such as Farlutal, Perlutex, and Gestapuran, among others.[132][10]

Society and culture

[edit]

Generic names

[edit]

Medroxyprogesterone acetate is the generic name of the drug and its INNTooltip INN, USANTooltip United States Adopted Name, BANTooltip BANM, and JANTooltip Japanese Accepted Name, while medrossiprogesterone is the DCITTooltip Denominazione Comune Italiana and médroxyprogestérone the DCFTooltip Dénomination Commune Française of its free alcohol form.[224][11][132][240][10] It is also known as 6α-methyl-17α-acetoxyprogesterone (MAP) or 6α-methyl-17α-hydroxyprogesterone acetate.[224][11][132][10]

Brand names

[edit]

MPA is marketed under a large number of brand names throughout the world.[10][11][132] Its most major brand names are Provera as oral tablets and Depo-Provera as an aqueous suspension for intramuscular injection.[10][11][132] A formulation of MPA as an aqueous suspension for subcutaneous injection is also available in the United States under the brand name Depo-SubQ Provera 104.[10][11] Other brand names of MPA formulated alone include Farlutal and Sayana for clinical use and Depo-Promone, Perlutex, Promone-E, and Veramix for veterinary use.[10][11][132] In addition to single-drug formulations, MPA is marketed in combination with the estrogens CEEs, estradiol, and estradiol valerate.[10][11][132] Brand names of MPA in combination with CEEs as oral tablets in different countries include Prempro, Premphase, Premique, Premia, and Premelle.[10][11][132] Brand names of MPA in combination with estradiol as oral tablets include Indivina and Tridestra.[10][11][132]

Availability

[edit]

Oral MPA and DMPA are widely available throughout the world.[10] Oral MPA is available both alone and in combination with the estrogens CEEs, estradiol, and estradiol valerate.[10] DMPA is registered for use as a form of birth control in more than 100 countries worldwide.[18][19][10] The combination of injected MPA and estradiol cypionate is approved for use as a form of birth control in 18 countries.[18]

United States

[edit]
See also: List of progestogens available in the United States

As of November 2016, MPA is available in the United States in the following formulations:[63]

  • Oral pills: Amen, Curretab, Cycrin, Provera – 2.5 mg, 5 mg, 10 mg
  • Aqueous suspension for intramuscular injection: Depo-Provera – 150 mg/mL (for contraception), 400 mg/mL (for cancer)
  • Aqueous suspension for subcutaneous injection: Depo-SubQ Provera 104 – 104 mg/0.65 mL (for contraception)

It is also available in combination with an estrogen in the following formulations:

  • Oral pills: CEEs and MPA (Prempro, Prempro (Premarin, Cycrin), Premphase (Premarin, Cycrin 14/14), Premphase 14/14, Prempro/Premphase) – 0.3 mg / 1.5 mg; 0.45 mg / 1.5 mg; 0.625 mg / 2.5 mg; 0.625 mg / 5 mg

While the following formulations have been discontinued:

  • Oral pills: ethinylestradiol and MPA (Provest) – 50 μg / 10 mg
  • Aqueous suspension for intramuscular injection: estradiol cypionate and MPA (Lunelle) – 5 mg / 25 mg (for contraception)

The state of Louisiana permits sex offenders to be given MPA.[241]

Generation

[edit]

Progestins in birth control pills are sometimes grouped by generation.[242][243] While the 19-nortestosterone progestins are consistently grouped into generations, the pregnane progestins that are or have been used in birth control pills are typically omitted from such classifications or are grouped simply as "miscellaneous" or "pregnanes".[242][243] In any case, based on its date of introduction in such formulations of 1964, MPA could be considered a "first-generation" progestin.[244]

Controversy

[edit]

Outside the United States

[edit]
  • In 1994, when DMPA was approved in India, India's Economic and Political Weekly reported that "The FDA finally licensed the drug in 1990 in response to concerns about the population explosion in the third world and the reluctance of third world governments to license a drug not licensed in its originating country."[245] Some scientists and women's groups in India continue to oppose DMPA.[246] In 2016, India introduced DMPA depo-medroxyprogesterone IM preparation in the public health system.[247]
  • The Canadian Coalition on Depo-Provera, a coalition of women's health professional and advocacy groups, opposed the approval of DMPA in Canada.[248] Since the approval of DMPA in Canada in 1997, a $700 million class-action lawsuit has been filed against Pfizer by users of DMPA who developed osteoporosis. In response, Pfizer argued that it had met its obligation to disclose and discuss the risks of DMPA with the Canadian medical community.[249]
  • Clinical trials for this medication regarding women in Zimbabwe were controversial with regard to human rights abuses and Medical Experimentation in Africa.
  • A controversy erupted in Israel when the government was accused of giving DMPA to Ethiopian immigrants without their consent. Some women claimed they were told it was a vaccination. The Israeli government denied the accusations but instructed the four health maintenance organizations to stop administering DMPA injections to women "if there is the slightest doubt that they have not understood the implications of the treatment".[250]

United States

[edit]

There was a long, controversial history regarding the approval of DMPA by the U.S. Food and Drug Administration. The original manufacturer, Upjohn, applied repeatedly for approval. FDA advisory committees unanimously recommended approval in 1973, 1975 and 1992, as did the FDA's professional medical staff, but the FDA repeatedly denied approval. Ultimately, on 29 October 1992, the FDA approved DMPA for birth control, which had by then been used by over 30 million women since 1969 and was approved and being used by nearly 9 million women in more than 90 countries, including the United Kingdom, France, Germany, Sweden, Thailand, New Zealand and Indonesia.[251] Points in the controversy included:

  • Animal testing for carcinogenicity – DMPA caused breast cancer tumors in dogs. Critics of the study claimed that dogs are more sensitive to artificial progesterone, and that the doses were too high to extrapolate to humans. The FDA pointed out that all substances carcinogenic to humans are carcinogenic to animals as well, and that if a substance is not carcinogenic it does not register as a carcinogen at high doses. Levels of DMPA which caused malignant mammary tumors in dogs were equivalent to 25 times the amount of the normal luteal phase progesterone level for dogs. This is lower than the pregnancy level of progesterone for dogs, and is species-specific.[252]
    DMPA caused endometrial cancer in monkeys – 2 of 12 monkeys tested, the first ever recorded cases of endometrial cancer in rhesus monkeys.[253] However, subsequent studies have shown that in humans, DMPA reduces the risk of endometrial cancer by approximately 80%.[50][51][52]
    Speaking in comparative terms regarding animal studies of carcinogenicity for medications, a member of the FDA's Bureau of Drugs testified at an agency DMPA hearing, "...Animal data for this drug is more worrisome than any other drug we know of that is to be given to well people."
  • Cervical cancer in Upjohn/NCI studies. Cervical cancer was found to be increased as high as 9-fold in the first human studies recorded by the manufacturer and the National Cancer Institute.[254] However, numerous larger subsequent studies have shown that DMPA use does not increase the risk of cervical cancer.[255][256][257][258][259]
  • Coercion and lack of informed consent. Testing or use of DMPA was focused almost exclusively on women in developing countries and poor women in the United States,[260] raising serious questions about coercion and lack of informed consent, particularly for the illiterate[261] and for mentally disabled people, who in some reported cases were given DMPA long-term for reasons of "menstrual hygiene", although they were not sexually active.[262]
  • Atlanta/Grady Study – Upjohn studied the effect of DMPA for 11 years in Atlanta, mostly on black women who were receiving public assistance, but did not file any of the required follow-up reports with the FDA. Investigators who eventually visited noted that the studies were disorganized. "They found that data collection was questionable, consent forms and protocol were absent; that those women whose consent had been obtained at all were not told of possible side effects. Women whose known medical conditions indicated that use of DMPA would endanger their health were given the shot. Several of the women in the study died; some of cancer, but some for other reasons, such as suicide due to depression. Over half the 13,000 women in the study were lost to followup due to sloppy record keeping." Consequently, no data from this study was usable.[260]
  • WHO Review – In 1992, the WHO presented a review of DMPA in four developing countries to the FDA. The National Women's Health Network and other women's organizations testified at the hearing that the WHO was not objective, as the WHO had already distributed DMPA in developing countries. DMPA was approved for use in United States on the basis of the WHO review of previously submitted evidence from countries such as Thailand, evidence which the FDA had deemed insufficient and too poorly designed for assessment of cancer risk at a prior hearing.
  • The Alan Guttmacher Institute has speculated that United States approval of DMPA may increase its availability and acceptability in developing countries.[260][263]
  • In 1995, several women's health groups asked the FDA to put a moratorium on DMPA, and to institute standardized informed consent forms.[264]

Research

[edit]

DMPA was studied by Upjohn for use as a progestogen-only injectable contraceptive in women at a dose of 50 mg once a month but produced poor cycle control and was not marketed for this use at this dosage.[265] A combination of DMPA and polyestradiol phosphate, an estrogen and long-lasting prodrug of estradiol, was studied in women as a combined injectable contraceptive for use by intramuscular injection once every three months.[266][267][268]

High-dose oral and intramuscular MPA monotherapy has been studied in the treatment of prostate cancer but was found to be inferior to monotherapy with cyproterone acetate or diethylstilbestrol.[269][270][271] High-dose oral MPA has been studied in combination with diethylstilbestrol and CEEs as an addition to high-dose estrogen therapy for the treatment of prostate cancer in men, but was not found to provide better effectiveness than diethylstilbestrol alone.[272]

DMPA has been studied for use as a potential male hormonal contraceptive in combination with the androgens/anabolic steroids testosterone and nandrolone (19-nortestosterone) in men.[273] However, it was never approved for this indication.[273]

MPA was investigated by InKine Pharmaceutical, Salix Pharmaceuticals, and the University of Pennsylvania as a potential anti-inflammatory medication for the treatment of autoimmune hemolytic anemia, Crohn's disease, idiopathic thrombocytopenic purpura, and ulcerative colitis, but did not complete clinical development and was never approved for these indications.[274][275] It was formulated as an oral medication at very high dosages, and was thought to inhibit the signaling of proinflammatory cytokines such as interleukin 6 and tumor necrosis factor alpha, with a mechanism of action that was said to be similar to that of corticosteroids.[274][275] The formulation of MPA had the tentative brand names Colirest and Hematrol for these indications.[274]

MPA has been found to be effective in the treatment of manic symptoms in women with bipolar disorder.[276]

Veterinary use

[edit]

MPA has been used to reduce aggression and spraying in male cats.[277] It may be particularly useful for controlling such behaviors in neutered male cats.[277] The medication can be administered in cats as an injection once per month.[277]

See also

[edit]

References

[edit]
Revisions and contributorsEdit on WikipediaRead on Wikipedia

Medroxyprogesterone acetate

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Medroxyprogesterone acetate (MPA) is a synthetic progestin and the 17α-acetate of , chemically known as pregn-4-ene-3,20-dione, 17-(acetyloxy)-6-methyl-,(6α)-. It acts as a potent agonist of the , mimicking the effects of endogenous progesterone to inhibit secretion, suppress , thicken cervical mucus, and alter the . MPA is administered in oral tablets (typically 2.5 to 10 mg doses) or long-acting intramuscular/subcutaneous injections (such as 150 mg every three months as Depo-Provera for contraception), making it a highly effective reversible contraceptive with a under 1% in typical use. Key indications include secondary amenorrhea, due to ovulatory dysfunction, prevention of in therapy, and adjunctive treatment for and . Despite its efficacy, MPA use is associated with significant adverse effects, including menstrual irregularities affecting over half of users in the first year, average of about 3 kg, and decreased density that may not fully reverse after discontinuation, prompting recommendations for monitoring in long-term users. Controversies include evidence of modestly elevated risk among current users (potentially 1.1- to 2.2-fold depending on duration and recency), possible increased acquisition risk due to immunosuppressive effects on genital mucosa, and recent associations with brain tumors in prolonged users. These risks underscore the need for individualized assessment, balancing benefits against empirical data on long-term harms.

Medical Uses

Contraception

Medroxyprogesterone acetate (MPA) serves as a progestin-only long-acting reversible contraceptive when administered as a 150 mg under the brand name Depo-Provera. The recommended dosing schedule involves repeat injections every 12 to 13 weeks to maintain contraceptive efficacy, with administration typically in the deltoid or gluteal muscle. This formulation provides sustained release of MPA, ensuring hormone levels sufficient for pregnancy prevention over the interval. With perfect use—defined as timely administration of injections every 13 weeks—the is less than 1 per 100 women in the first year. In typical use, accounting for occasional delays in scheduling injections, the rises to approximately 4 to 6 pregnancies per 100 women annually, based on large-scale observational data from clinical practice. These rates derive from studies tracking unintended pregnancies among users, highlighting the method's reliability when adherence to the injection timeline is maintained. The primary mechanism involves suppression of secretion from the pituitary, which inhibits follicular development and in nearly all cycles. Secondary effects include thickening of cervical mucus to impede migration and thinning of the to reduce receptivity for implantation. These actions collectively prevent fertilization and , with inhibition confirmed in pharmacokinetic studies showing sustained MPA concentrations above thresholds for suppression (approximately 0.1 ng/mL). As a progestin-only method, Depo-Provera avoids estrogen-related vascular risks, making it suitable for women with contraindications to combined hormonal contraceptives, such as those with a history of or . It requires no daily user action, reducing compliance errors compared to oral progestin-only pills, which exhibit typical-use failure rates of about 9% due to missed doses. This quarterly dosing supports higher real-world effectiveness, with failure rates roughly half those of progestin-only orals in comparative analyses.

Hormone Replacement Therapy

Medroxyprogesterone acetate (MPA) is employed in with in () for postmenopausal women with an intact primarily to counteract the proliferative effects of unopposed on the , thereby reducing the incidence of and associated risk. Common regimens include continuous combined therapy with oral MPA at 2.5 to 5 mg daily alongside , or sequential cyclic administration of 5 to 10 mg daily for 12 to 14 days per month. Clinical trials demonstrate that these doses provide adequate endometrial protection, with continuous 2.5 mg MPA achieving amenorrhea in approximately 80% of women by six months and effectively suppressing in with conjugated equine estrogens (CEE). In the (WHI) trial, which evaluated CEE 0.625 mg plus MPA 2.5 mg continuously in over 16,000 postmenopausal women, the regimen significantly lowered incidence compared to , confirming progestin's protective role against estrogen-induced changes. However, the same trial reported a 24% to 28% increased relative risk of invasive with combined therapy versus after 5.6 years of follow-up, with risk declining post-discontinuation. This elevation in breast cancer risk contrasts with estrogen-alone therapy in hysterectomized women, which showed no increase or a slight reduction. Combined estrogen-MPA therapy effectively alleviates menopausal symptoms, reducing frequency by 70% to 90% within one month, comparable to estrogen monotherapy but with added endometrial safeguarding. Progestin-only MPA at lower HRT doses offers limited relief compared to the combination, underscoring 's primary role in symptom control. In perimenopausal contexts, MPA aids in managing through cyclic dosing to induce withdrawal, while for secondary amenorrhea, 5 to 10 mg daily for 5 to 10 days induces secretory transformation and bleeding to assess ovarian function.

Gynecological Disorders

Medroxyprogesterone acetate (MPA) serves as a progestin for (AUB), especially in ovulatory or anovulatory dysfunctional cases driven by unopposed , which promotes endometrial proliferation and irregular shedding. Administered orally at doses of 5 to 10 mg daily for 10 to 14 days, MPA counters estrogen effects by inducing secretory transformation of the , culminating in organized withdrawal bleeding that stabilizes menstrual cycles and diminishes blood loss. The American College of Obstetricians and Gynecologists (ACOG) guidelines position MPA as a primary medical option for acute in stable reproductive-aged women, recommending multidose regimens to achieve before transitioning to cyclic maintenance. Clinical data indicate MPA's effectiveness in acute settings, with bleeding cessation in 76% of women within a of 3 days in comparative trials against combined oral contraceptives. For adolescents with heavy , high-dose oral MPA (e.g., 20 mg every 8 hours initially) combined with depot injections has resolved symptoms in over 80% of cases within days, per prospective evaluations, though response varies with bleeding duration exceeding 10 days potentially reducing efficacy. Cyclic use for ongoing regulation yields short-term success rates of 70% to 90% in halting irregular and normalizing patterns, as observed in cohort studies of premenopausal women, with monitoring advised to limit duration and prevent prolonged amenorrhea. In , MPA mitigates and chronic by exerting progestational suppression on ectopic endometrial tissue, fostering and reducing inflammatory responses. Oral regimens at 10 to 50 mg daily for 3 months have shown symptom relief in randomized controlled trials among infertile women, with follow-up assessments confirming sustained benefits at 6 months without fertility impairment post-treatment. Depot MPA injections further demonstrate equivalence to other progestins in reduction up to 3 years post-surgery in comparative RCTs, offering a cost-effective alternative with minimal differences in recurrence rates. Guidelines across multiple societies endorse MPA for endometriosis-associated , emphasizing short-term application with efficacy rates exceeding 80% for symptom control, though long-term data prioritize reversible options to preserve bone . Treatment response requires via symptom scores and , with discontinuation after 3 to 6 months to assess persistence.

Oncology Applications

Medroxyprogesterone acetate (MPA) has been employed in high-dose oral regimens, typically 400 to 1000 mg per day, for the palliative management of advanced hormone-sensitive cancers including endometrial carcinoma, , and . In advanced or recurrent endometrial cancer, progestin therapies like MPA yield objective response rates of approximately 30%, with clinical benefit rates up to 52% in meta-analyses of randomized trials, though complete responses are less common in non-fertility-sparing contexts. For metastatic , MPA has demonstrated partial tumor regressions in subsets of patients, with historical series reporting objective responses in 10 to 20% of cases treated palliatively. In postmenopausal women with advanced , high-dose MPA achieves response rates of 20 to 30% in soft tissue and visceral metastases, particularly when prior endocrine therapies have failed. Beyond direct antitumor effects via progestogenic mechanisms, MPA's glucocorticoid-like activity contributes to stimulation and reversal of in terminal cancer patients. Phase III trials and double-blind placebo-controlled studies have shown significant improvements in scores and food intake with high-dose MPA (e.g., 500-1000 mg/day), leading to average weight gains of 2 to 4 kg over 4 to 6 weeks in anorexic patients with advanced malignancies. These effects enhance metrics in palliative settings, though without extending overall survival in meta-analyses of progestin trials for anorexia-cachexia syndrome. MPA received U.S. approval for palliative use in advanced endometrial and s in the late 1950s to early 1960s, based on early evidence of tumor regression and symptom control. Its application lacks curative intent, focusing instead on temporary disease stabilization and palliation, and has diminished in favor of targeted therapies like tyrosine kinase inhibitors for or anti-HER2 agents for since the 1990s.

Other Therapeutic Indications

Medroxyprogesterone acetate (MPA) has been investigated off-label in high doses for appetite stimulation and weight gain in non-oncologic , such as HIV-associated . In HIV-infected patients, adjunctive MPA at doses of 500 mg daily orally enhanced the efficacy of protein-rich nutritional support, leading to improved body weight and utilization compared to alone. Progestogens like MPA promote weight gain through central mechanisms involving stimulation in the , with clinical trials reporting average increases of 5 to 10% in body weight over 4 to 12 weeks in cachectic patients, though evidence remains limited to small studies outside . Use in primary is not established as standard, with most data derived from contexts rather than eating disorders per se. MPA has been employed historically for managing paraphilic disorders and reducing in male sex offenders via antiandrogenic effects. High-dose intramuscular MPA (typically 200-400 mg weekly) suppresses serum testosterone levels substantially, often by over 80%, thereby diminishing sexual fantasies, arousal, and deviant behaviors in responsive individuals. Small cohort studies and reviews indicate treatment response in 70-90% of motivated patients, with reduced urges within 3 weeks, though long-term adherence is required and efficacy wanes upon discontinuation; modern alternatives like GnRH agonists have largely supplanted MPA due to better tolerability profiles. Limited evidence from randomized controlled trials supports adjunctive MPA for mood stabilization in refractory mania. In a four-week RCT of 32 patients with persistent manic symptoms despite or , oral MPA 30 mg daily accelerated symptom resolution, with greater reductions in Young Mania Rating Scale scores compared to (effect size 0.8), potentially via modulation of limbic androgen receptors. Such use remains investigational and not first-line, confined to cases unresponsive to standard antipsychotics or mood stabilizers.

Safety and Adverse Effects

Contraindications and Precautions

Medroxyprogesterone acetate (MPA) is contraindicated in patients with known or suspected , as it may cause fetal harm including masculinization of fetuses when administered during the first trimester. It is also contraindicated in cases of undiagnosed abnormal , due to the risk of masking underlying endometrial pathology. Active or history of represents an absolute , given MPA's progestogenic activity potentially stimulating hormonally sensitive tumors. Severe hepatic impairment or active precludes use, as MPA is metabolized by the liver and may exacerbate dysfunction or cause . Relative contraindications include current or past thromboembolic disorders, , or active , where the risk of recurrence or exacerbation must be weighed against benefits, as progestins can influence factors. Patients with with aura, uncontrolled , or with vascular complications require careful evaluation, with guidelines recommending risk-benefit assessment due to potential cardiovascular events observed in observational data. Precautions are essential for adolescents and young adults using injectable MPA formulations for contraception, as prolonged use is associated with significant bone mineral density (BMD) loss—up to 5-7% at the lumbar spine after 2 years in studies of depot medroxyprogesterone acetate (DMPA)—necessitating baseline and periodic BMD monitoring via (DEXA) scans per FDA recommendations. Women over 35 who smoke more than 15 cigarettes daily face heightened cardiovascular risks, with cohort studies reporting elevated rates of and in progestin users; initiation or continuation should involve counseling. Screening protocols prior to initiation include evaluation for contraindications via and physical exam, with baseline lipid profiles and coagulation studies advised in patients with risk factors for or to guide ongoing monitoring.

Common Side Effects

In clinical trials for medroxyprogesterone acetate (MPA) injectable suspension (Depo-Provera CI) used for contraception, the most common adverse effects included menstrual irregularities, with bleeding or spotting reported in 57% of women at 12 months, decreasing to 32% at 24 months, and amenorrhea in 55% at 12 months, rising to 68% at 24 months. These disruptions typically diminish over time as users transition to amenorrhea, though initial spotting remains a leading cause of discontinuation in the first year. Weight gain affects a substantial portion of users, with 38% gaining more than 10 pounds after 24 months; average gains were 5.4 pounds at 1 year and 8.1 pounds at 2 years in large-scale studies. Headaches occurred in 17% of trial participants, or discomfort in 11%, and nervousness in 11%. Mood changes, such as depression, were less frequent, affecting 1% to 5% of users. Injection-site reactions, including pain, lumps, or dimpling, arise primarily from inadvertent and were noted in post-marketing surveillance, though incidence was low (under 5%); these are dose- and technique-dependent, with proper minimizing occurrence. Many common effects, including menstrual changes and headaches, show empirical resolution in over 80% of cases upon discontinuation or as tolerance develops, based on cohort data from millions of users tracked via . Management of persistent spotting may involve nonsteroidal anti-inflammatory drugs (NSAIDs) to reduce prostaglandin-mediated bleeding, though efficacy varies by individual.

Serious and Long-Term Risks

Use of depot medroxyprogesterone acetate (DMPA), a common injectable form of medroxyprogesterone acetate, has been associated with an increased risk of venous thromboembolism (VTE), with meta-analyses reporting relative risks of approximately 2- to 2.6-fold compared to non-users after adjustment for confounders such as age, smoking, and . This elevation appears specific to DMPA among progestin-only contraceptives and is attributed to potential prothrombotic effects of medroxyprogesterone acetate on coagulation factors, though absolute risks remain low in otherwise healthy women. Long-term DMPA use is linked to reductions in bone mineral density (BMD), with longitudinal studies using (DEXA) scans documenting losses of 5.7% to 7.5% at the lumbar spine and after 2 or more years of injections. These deficits occur primarily in the first 2 years and are partially reversible upon discontinuation, with recovery of 50% to 80% of lost BMD observed within 2 to 5 years in adolescents and adults, though full restoration may not occur in all cases, particularly with prolonged prior exposure. The mechanism involves suppression of levels due to MPA's antigonadotropic effects, mimicking a hypoestrogenic state that accelerates . Recent studies have identified an elevated risk of with prolonged MPA exposure, including DMPA, with a national case-control analysis reporting a of 2.43 (95% CI 1.77-3.33) for ever-use and higher odds (up to 3- to 5-fold) for cumulative doses exceeding 1 year or equivalent. A 2024 French similarly found increased intracranial incidence with extended medroxyprogesterone acetate use, prompting regulatory updates on risk minimization. This association may stem from MPA's high-affinity binding to progesterone receptors, which are expressed in tissue, potentially promoting tumorigenesis via non-genomic signaling pathways. Evidence on risk is inconsistent but suggests a modest elevation with recent or long-term MPA use, particularly in combined hormone therapies; the reported a of 1.24 (absolute risk increase of 8 cases per 10,000 women-years) for plus MPA versus . For DMPA alone, some case-control studies indicate a 2.2-fold risk with 12 or more months of recent use, though this may be confounded by surveillance bias, as users undergo more frequent breast examinations. Other analyses, including cohort data on injectable progestogens, show no significant increase (RR 0.9), highlighting the need for beyond observational associations.

Reproductive and Infectious Disease Considerations

The Evidence for Contraceptive Options and Outcomes (ECHO) trial, a 2019 involving approximately 7,800 women in , compared incidence rates among users of intramuscular depot medroxyprogesterone acetate (DMPA-IM), copper intrauterine devices, and levonorgestrel implants, finding no statistically significant difference overall (3.81 cases per 100 woman-years for DMPA-IM versus comparators).31288-7/fulltext) However, prior observational data from , including individual participant data meta-analyses of studies involving over 39,000 women, have reported a 40-50% relative increase in acquisition risk associated with DMPA use compared to non-users or other methods, potentially confounded by factors such as sexual behavior or healthcare-seeking patterns. Laboratory studies, including a 2025 analysis of cervical secretions from DMPA-treated women, indicate that MPA exposure may enhance infectivity by altering mucosal factors that facilitate viral entry and replication in target cells. Despite these associations, causality remains unproven due to inconsistencies between randomized and observational evidence, with potential biological mechanisms involving or epithelial changes not fully resolving the debate. The , in updated 2019 guidelines, recommends that women in high HIV-prevalence areas may continue DMPA-IM with appropriate counseling on risks and use, citing the substantial benefits of preventing unintended pregnancies as outweighing uncertain risks in contexts where alternatives are limited. Data on other sexually transmitted infections are mixed; observational studies, such as one involving 819 women, have linked DMPA to higher rates of and acquisition, possibly due to progestin-induced thinning of increasing susceptibility, though randomized evidence shows no consistent elevation and questions the role of simple mucosal disruption.00049-9/fulltext) Medroxyprogesterone acetate is classified as FDA X, contraindicated during pregnancy due to risks of fetal harm, including potential such as clitoral enlargement in female fetuses exposed early in .

Pharmacology

Pharmacodynamics

Medroxyprogesterone acetate (MPA) acts primarily as a potent at the progesterone receptors PR-A and PR-B, binding with high affinity comparable to or exceeding that of progesterone in various assays, thereby mimicking the effects of endogenous progesterone on target tissues. This activation inhibits (GnRH) pulsatility and directly suppresses pituitary secretion of (LH) and (FSH), achieving profound antigonadotropic effects that reduce LH and FSH levels by over 60-90% depending on dose and formulation in reproductive models. These actions stem from PR-mediated on the hypothalamic-pituitary-gonadal axis, as demonstrated in pituitary cell cultures and animal models where MPA dose-dependently blunts gonadotropin release. MPA exhibits partial agonist activity at the (AR), with binding affinity sufficient to elicit androgenic responses , such as in AR-transfected cell lines, though weaker than . This AR interaction, observed in cells and models, may underlie certain physiological effects like or at specific doses. Similarly, MPA binds the (GR) with substantial relative binding affinity (approximately 40-50% of or dexamethasone in receptor binding studies), promoting GR translocation and gene transcription that dissociates anti-inflammatory effects from full mineralocorticoid or catabolic actions. At high doses, this GR agonism contributes to suppression by inhibiting (ACTH)-stimulated production, as evidenced in adrenal cell assays and animal studies showing reduced output. In addition to nuclear receptor actions, MPA modulates neurosteroid-sensitive ion channels, positively allosteric modulating specific GABA_A receptor subtypes (e.g., α1β2γ2 and α4β3δ configurations) in heterologous expression systems and native hypothalamic neurons, enhancing chloride influx and inhibitory neurotransmission akin to endogenous neurosteroids. This GABA_A potentiation, observed at nanomolar concentrations, supports anxiolytic-like effects in behavioral models independent of PR activation. MPA also directly inhibits steroidogenic enzymes, competitively blocking 3β-hydroxysteroid dehydrogenase and 17α-hydroxylase/17,20-lyase activities in human gonadal and adrenal microsomes, thereby suppressing de novo synthesis of androgens, estrogens, and corticosteroids beyond pituitary-mediated pathways. Unlike certain progestins with mixed profiles, MPA demonstrates negligible binding to or activation of estrogen receptors, lacking intrinsic estrogenic activity in uterine or breast cell proliferation assays and instead antagonizing estrogen-driven responses via PR crosstalk.

Pharmacokinetics

Medroxyprogesterone acetate (MPA) exhibits route-dependent pharmacokinetics, with rapid absorption following oral administration and prolonged release from intramuscular (IM) or subcutaneous (SC) depot formulations. Oral MPA tablets are rapidly absorbed from the gastrointestinal tract, achieving maximum plasma concentrations within 2 to 4 hours post-dose, with a bioavailability approaching 90-100%. The biological half-life of oral MPA is approximately 40 to 60 hours. In contrast, IM administration of 150 mg MPA as an aqueous suspension (Depo-Provera) results in peak plasma levels at 1 to 2 weeks, followed by a gradual decline, with plasma concentrations remaining detectable for 4 to 6 months. Therapeutic plasma levels for contraception are typically maintained at 1 to 5 ng/mL, with suppression occurring above approximately 0.5 ng/mL. Depot formulations achieve steady-state conditions after 3 to 6 months of repeated dosing every 12 to 13 weeks, though single-dose profiles show an elimination of 40 to 50 days. MPA is extensively bound to plasma proteins (about 90%), primarily and corticosteroid-binding . MPA undergoes hepatic metabolism primarily via () to hydroxylated and other inactive metabolites. These metabolites, along with unchanged drug, are excreted mainly in the , with at least 11 metabolites identified. SC administration of 104 mg MPA (depo-subQ Provera) yields similar profiles to IM, with maximum concentrations reached within days and sustained levels above 0.2 ng/mL for several months. Formulation differences, such as aqueous suspension versus microcrystalline, influence absorption rates but not overall in depot use.

Chemistry and Synthesis

Chemical Structure

Medroxyprogesterone acetate (MPA) is a synthetic progestin with the systematic name (6α,17α)-17-(acetyloxy)-6-methylpregn-4-ene-3,20-dione. Its molecular formula is C24H34O4, and it has a molecular weight of 386.53 g/mol. Structurally, MPA is derived from progesterone (pregn-4-ene-3,20-dione) through the introduction of a at the 6α position and an at the 17α position of the skeleton. The 6α-methylation reduces susceptibility to rapid hepatic , thereby improving oral compared to progesterone, while the 17α-acetoxy modification enhances progestogenic potency and stability. MPA exhibits lipophilic properties, being practically insoluble in water but soluble in organic solvents such as chloroform and acetone, which facilitates its for sustained-release depot injections. This physicochemical profile supports its administration in oral doses ranging from 2.5 to 10 mg and intramuscular suspensions at concentrations up to 150 mg/mL.

Synthesis and Formulations

Medroxyprogesterone acetate is produced semisynthetically from progesterone through chemical modifications that introduce a methyl group at the 6α-position and an acetate ester at the 17α-hydroxy group. The process typically starts with 17α-hydroxyprogesterone as a key intermediate, which undergoes catalytic methylation—often involving p-toluenesulfonic acid or similar agents in alcoholic solvents—followed by acetylation to yield the final compound. This route, refined for scalability in the 1950s, relies on established steroid chemistry techniques enabling efficient industrial production from plant-derived precursors like diosgenin. Pharmaceutical formulations of medroxyprogesterone acetate include oral tablets in strengths of 2.5 mg, 5 mg, 10 mg, and 100 mg for daily administration, as well as injectable suspensions for depot delivery. The intramuscular formulation Depo-Provera consists of 150 mg/mL or 400 mg/mL microcrystalline suspensions in aqueous vehicles, designed for deep injection to achieve sustained release over 12 to 13 weeks through slow dissolution of the crystals, which maintains therapeutic plasma levels for contraception or other indications. A subcutaneous option, Depo-subQ Provera 104, provides 104 mg/0.65 mL in a prefilled for self-administration, with comparable to the intramuscular version. Generic formulations have proliferated post-patent expiry, with the U.S. requiring via pharmacokinetic studies showing comparable area under the curve and maximum concentrations for oral forms, alongside assessments of particle size and suspension uniformity for injectables to ensure equivalent release profiles and stability. Test products must match reference listed drugs in qualitative and quantitative composition of active and inactive ingredients, with suspensions demonstrating consistent microcrystal morphology to replicate depot duration without altering .

History and Development

Early Research and Approval

Medroxyprogesterone acetate (MPA) was developed by the Upjohn Company in the through experimentation with synthetic progesterone analogs, initially for potential therapeutic uses beyond contraception. Its synthesis was first reported in , building on earlier microbial transformation techniques applied to steroid compounds to enhance progestational potency. Pre-clinical studies in the late confirmed MPA's strong progestin activity, prompting initial human investigations for gynecological disorders such as amenorrhea and dysfunctional uterine bleeding. Early clinical trials in the early evaluated oral MPA at doses of 5 to 10 mg daily, demonstrating efficacy in inducing withdrawal bleeding and restoring menstrual cycles in women with secondary amenorrhea, with response rates exceeding 80% in small cohorts. The U.S. (FDA) approved oral MPA on June 18, 1959, for treating secondary amenorrhea, due to hormonal imbalance, and endometrial . For injectable depot formulations (DMPA), initiated clinical trials in 1963 targeting long-acting contraception, with pivotal multicenter studies in the 1960s and involving thousands of women showing contraceptive efficacy rates of approximately 99.7% ( of 0.3 pregnancies per 100 woman-years at 150 mg every 90 days). However, U.S. approval for this indication was delayed due to carcinogenicity findings in dogs, where high-dose administration induced mammary tumors, raising concerns about potential human risk despite lack of corroboration in rodents or initial human data. The endorsed DMPA for in developing countries during the , emphasizing its high efficacy and acceptability in resource-limited settings while noting the animal data limitations and need for ongoing monitoring.

Regulatory Milestones

Medroxyprogesterone acetate (MPA) received initial U.S. Food and Drug Administration (FDA) approval on June 18, 1959, for oral tablets in treating secondary amenorrhea and abnormal uterine bleeding. The injectable form was subsequently approved in the early 1960s for palliative management of advanced endometrial carcinoma and renal cell carcinoma. Approval for contraceptive use as depot medroxyprogesterone acetate (DMPA, branded Depo-Provera) faced significant delays despite applications dating to 1967, owing to concerns over animal studies indicating potential carcinogenicity, including mammary tumors in dogs and endometrial cancer in monkeys; full FDA approval for contraception occurred on October 29, 1992, following additional safety data. In contrast, European regulators granted earlier access for contraception. In the , MPA was licensed for short-term contraceptive use in limited circumstances, such as post-rubella vaccination or immediate postpartum, since 1978, with broader approvals following in the 1980s across countries including and . The (EMA) later harmonized oversight, including the 2004 subcutaneous formulation approval under Depo-SubQ Provera 104. Label updates addressed emerging risks. In November 2004, the FDA mandated a warning on Depo-Provera labeling, highlighting significant density loss with prolonged use (greater with duration exceeding two years) and advising against long-term contraception unless alternative methods are inadequate; similar warnings were implemented by EMA member states for risk. Pediatric use was restricted accordingly, with MPA deemed inappropriate before and long-term administration (>2 years) discouraged in adolescents due to irreversible bone effects, limiting approvals primarily to short-term contraception when benefits outweigh risks. Recent pharmacovigilance actions followed cohort studies linking prolonged high-dose MPA exposure to meningioma risk. In March 2024, a French nationwide study reported a 5.6-fold increased risk of intracranial meningioma with extended injectable use (≥12 months), prompting the Agence Nationale de Sécurité du Médicament (ANSM) and EMA's Pharmacovigilance Risk Assessment Committee (PRAC) to recommend updated contraindications, including avoidance of cumulative doses exceeding certain thresholds and immediate discontinuation upon meningioma diagnosis to permit potential tumor regression. By September 2024, EMA endorsed precautionary measures across the EU, echoed in national agencies like the UK's MHRA via direct healthcare communications in October 2024, emphasizing screening for meningioma history before initiation. Off-label uses, such as for gender dysphoria suppression, faced heightened scrutiny, with regulators reinforcing adherence to approved indications amid these updates.

Key Clinical Trials

One of the earliest large-scale evaluations of medroxyprogesterone acetate (MPA) for contraception involved multicenter trials in the , including a study by seven investigators administering 300 mg intramuscular injections every six months to over 5,000 women, which reported a of approximately 0.3 per 100 woman-years, confirming high comparable to other long-acting methods. Subsequent U.S. trials in the mid-1970s, such as those supporting FDA approval for Depo-Provera in for non-contraceptive uses (with contraceptive approval following in the ), similarly demonstrated failure rates below 1 per 100 woman-years in adherent users, though with noted delays in return averaging 9-12 months post-discontinuation. In hormone replacement therapy (HRT), the Women's Health Initiative (WHI) randomized controlled trial (1990s enrollment, primary results 2002) assessed conjugated equine estrogens (CEE) plus 2.5 mg daily oral MPA in 16,608 postmenopausal women aged 50-79, finding no overall reduction in coronary heart disease (hazard ratio [HR] 1.24 for the first year, neutral thereafter) but a 2-fold increased risk of venous thromboembolism (VTE; HR 2.06, 95% CI 1.59-2.67), including deep vein thrombosis and pulmonary embolism, primarily in the initial years of use. The trial's CEE+MPA arm was halted early after 5.6 years due to excess breast cancer events, though cardiovascular neutrality held across subgroups without early initiation bias. Longitudinal cohort studies from 2006-2010 quantified MPA's impact on density (BMD) in adolescents and young adults using depot MPA (DMPA). A prospective study of 146 DMPA users aged 12-18 measured (DXA) at baseline and annually, reporting mean BMD losses of 1.3-1.5% per year at the lumbar spine and over 2 years, compared to gains in non-users, with partial recovery (up to 80% of loss regained) within 2 years post-discontinuation in follow-up data. These findings, corroborated in similar cohorts, informed FDA black-box warnings on DMPA-related bone loss, emphasizing monitoring in long-term users under age 18. For , phase III trials in the 1980s evaluated high-dose MPA in advanced endometrial . The Gynecologic Oncology Group (GOG) conducted a randomized dose-response study comparing 1,000 mg/day versus 200 mg/day oral MPA in 145 women with measurable disease, showing objective response rates of 25-30% (complete plus partial) and of 3-5 months in responders, with higher doses yielding marginally better outcomes but increased like fluid retention. In , phase II-III evaluations of high-dose MPA (e.g., 1 g/week initially) in metastatic patients reported response rates around 10-15% with median survival extensions of 4-6 months, though later meta-analyses questioned superiority over in unselected cohorts.

Society, Culture, and Regulation

Brand Names and Availability

Medroxyprogesterone acetate is marketed under the brand names Provera for oral tablets and Depo-Provera for intramuscular injectable suspension, both produced by . A subcutaneous injectable formulation is available as Depo-SubQ Provera 104, also by . Other brands include Cycrin and Curretab for oral use, though these are less common. Generic versions of acetate in oral, intramuscular, and subcutaneous forms are widely available following the expiration of original patents in the late , comprising the majority of supply in regulated markets. The drug is approved and distributed in over 90 countries outside the , with broad availability in , , , and through national regulatory agencies and international aid programs. Injectable formulations predominate in low-resource settings due to ease of administration and long duration, while oral tablets are more prevalent in high-income countries with established networks. In developing countries, costs for injectable doses are subsidized to approximately $1 per three-month dose via partnerships such as those between and the Bill & Melinda Gates Foundation, facilitating access through programs.

Usage Patterns and Access

Injectable formulations of medroxyprogesterone acetate, particularly depot medroxyprogesterone acetate (DMPA), serve primarily as a contraceptive in low- and middle-income countries, accounting for a substantial share of hormonal method use in sub-Saharan Africa and select Asian regions. In sub-Saharan Africa, injectables like DMPA represent about 36% of modern contraceptive methods among women, with a regional prevalence of 9.6% among those of reproductive age as of 2019. Usage equates to roughly 40% of all contraceptive methods in eastern and southern sub-Saharan countries, where it is the dominant reversible hormonal option. In Asia, prevalence exceeds 20% of contraceptive users in nations like Indonesia, though overall reliance is lower compared to sterilization. In high-income regions such as the and , DMPA adoption has decreased owing to preferences for alternatives like intrauterine devices and implants, alongside higher discontinuation linked to side effects including and concerns. Scandinavian and broader European data indicate persistently low user rates, with national registries showing downward trends in prescriptions since the early . Despite this, DMPA maintains steady uptake among patients prone to non-compliance with daily or user-dependent methods, benefiting from its three-month dosing interval that ensures high efficacy without frequent intervention. Among demographics, adolescents and teens disproportionately select DMPA for its superior effectiveness, with first-year typical-use failure rates of 0.3%, outperforming oral contraceptives. Studies of clinic populations show 43% of adolescent choosers opting for DMPA, often those with prior pregnancies seeking reliable long-acting protection. In low- and middle-income countries, access faces challenges from supply chain disruptions, including stockouts driven by inadequate procurement and distribution, which affect up to significant portions of facilities. Additionally, the requirement for trained personnel to perform intramuscular or subcutaneous injections limits scalability, particularly in remote areas lacking skilled providers. Efforts to introduce self-injection options aim to mitigate these barriers but remain constrained by training needs and policy implementation.

Economic and Market Aspects

The global market for medroxyprogesterone acetate (MPA) reached approximately $1.2 billion in 2024, with projections indicating sustained growth into 2025 primarily fueled by generic injectables and expanding access in developing regions. This valuation reflects the dominance of depot formulations like medroxyprogesterone acetate injectable suspension, which account for a significant share due to their role in long-acting reversible contraception amid rising demand for affordable options. Production and distribution of MPA underwent structural changes following the 2020 merger of Pfizer's business unit—original developer of Depo-Provera—with to form Inc., consolidating manufacturing of both branded and generic versions under a single entity focused on off-patent pharmaceuticals. This shift enhanced generic supply chains but required divestitures of certain injectable assets to address antitrust concerns, including medroxyprogesterone acetate solutions for uterine bleeding treatment. Generic production costs remain low, enabling retail prices for oral MPA as little as $0.12 per tablet and injectable doses under $1 in bulk procurement, far below original branded equivalents. Pharmacoeconomic analyses highlight MPA's cost-effectiveness, particularly for depot injections, which avert pregnancies at incremental societal costs of $15 per averted pregnancy or $98 per maternal disability-adjusted life year in self-administration models versus health-worker delivery. Subsidized pricing through partnerships like those between Pfizer, UNFPA, and donors has reduced per-dose costs to $0.85 for subcutaneous formulations such as Sayana Press, equating to roughly $3–4 annually for quarterly dosing and yielding substantial savings against unintended pregnancy expenses, estimated at over $10,000 per case in high-income settings. UNFPA procurement supports tens of millions of MPA vials yearly at these rates, facilitating distribution of over 23 million units of 150 mg medroxyprogesterone acetate in 2021 alone for global family planning programs.

Controversies and Debates

Historical Approval Disputes

In the United States, the Food and Drug Administration (FDA) delayed approval of depot medroxyprogesterone acetate (DMPA, branded as Depo-Provera) for contraceptive use throughout the 1970s due to mammary gland tumors observed in beagle dog studies conducted in the late 1960s. These studies administered MPA at doses equivalent to human contraceptive levels (approximately 150 mg every three months, scaled by body weight) and reported a dose-dependent increase in benign and malignant mammary tumors, including adenocarcinomas, in treated beagle bitches. In March 1978, the FDA formally denied Upjohn's application to market DMPA for contraception, determining that the animal carcinogenicity data outweighed available human evidence of safety, and mandating further long-term studies despite prior limited approvals for other indications like endometrial cancer treatment. Regulatory disputes centered on the predictive value of models, as subsequent analyses highlighted the breed's exceptional sensitivity to progestogens—manifesting high spontaneous rates (up to 25% in untreated beagles) exacerbated by hormonal exposure—without comparable effects in , rhesus monkeys, or early cohorts. No increased incidence was observed in rats or mice at similar relative doses, and epidemiological data from international users (millions of injections by the ) showed no elevated cancer signals, leading proponents to argue that beagle findings were species-specific artifacts rather than translatable risks. The FDA's insistence on additional data reflected a precautionary stance, though critics contended it unduly prioritized non-equivalent animal over accumulating clinical profiles from global use. Internationally, DMPA faced less stringent barriers, with approval for contraception granted in the United Kingdom as early as 1961 for short-term use in specific cases, such as postpartum or post-rubella vaccination women, predating U.S. concerns. The World Health Organization (WHO) endorsed DMPA for family planning in developing countries during the 1970s despite vocal opposition from feminist and animal rights groups, who cited the beagle data as evidence of potential human carcinogenicity and raised ethical issues around informed consent and coercion in low-resource settings. Resolution in favor of approval emphasized human equivalence studies and post-marketing surveillance, subordinating animal model discrepancies to longitudinal evidence of efficacy and safety in diverse populations.

Risk-Benefit Assessments

In contraceptive applications, depot medroxyprogesterone acetate (DMPA) exhibits failure rates under 1% with typical use, comparable to intrauterine devices and implants, thereby preventing unintended pregnancies that contribute to maternal mortality exceeding risks from alternative methods or non-use in observational models. Global decision analyses estimate that DMPA averts hundreds of thousands of unintended pregnancies annually in high-burden settings, reducing associated complications like unsafe abortions and , with net benefits persisting after accounting for documented side effects. Associated density reductions with DMPA use, averaging 5-7% over two years, prove largely reversible post-discontinuation, as evidenced by longitudinal cohorts showing near-full recovery within 2-3 years, mitigating long-term concerns in premenopausal users. For acquisition, randomized trials such as the ECHO study (2019) report no elevated incidence with DMPA versus copper IUDs or implants ( ≈1.0), contrasting observational associations potentially confounded by behavioral or access factors, thus questioning causal attributions from non-randomized data. In (HRT) for postmenopausal women with intact uteri, medroxyprogesterone acetate provides endometrial opposition to unopposed , slashing incidence from 20-30% to under 1% in trials, with number-needed-to-treat estimates of 10-20 to avert one case of complex over 1-2 years. This protective effect offsets a 1.5-2-fold relative increase in venous thromboembolism (VTE) risk (absolute incidence 2-4 per 1,000 user-years in combined regimens), particularly favoring short-term use in low-risk cohorts per risk-benefit modeling, where endometrial cancer prevention yields superior outcomes. Overemphasis on VTE in certain guidelines has been critiqued for relying on older observational cohorts with higher baseline risks, underweighting RCT-derived absolute benefits in screened populations.

Recent Evidence on Meningioma and Other Tumors

A nationwide case-control study in published in 2024 analyzed 18,061 women undergoing between 2009 and 2018, matched to 90,305 controls without , and found that prolonged use (more than 12 months' cumulative exposure) of medroxyprogesterone acetate (MPA) was associated with an adjusted (OR) of 5.55 (95% CI 2.27-13.56) for intracranial requiring . This risk was dose-dependent, with higher cumulative doses correlating to greater odds, particularly for injectable depot formulations used for contraception or treatment. The association parallels prior observations with high-dose , another potent progestin with strong agonism, which has shown risks up to 20-fold in long-term users due to presumed promotion of via hormonal pathways. linked to progestins are typically benign (WHO grade 1), yet often necessitate surgical resection due to symptoms from , with recurrence risks post-resection. In contrast to these meningioma signals, recent pharmacoepidemiologic data on MPA's association with breast cancer indicate neutrality or minimal long-term elevation. A 2023 systematic review of seven cohort studies reported no overall increased breast cancer incidence among depot MPA users (relative risks ranging 0.7-1.2), though a transient elevation may occur in current or recent users, dissipating after discontinuation; this debunks early concerns of substantial oncogenic risk from progestin-only contraceptives. For endometrial cancer, meta-analyses affirm MPA's protective role, as progestins counteract estrogen-induced endometrial proliferation; continuous combined estrogen-progestin regimens, including those with MPA, have shown statistically lower incidence compared to unopposed estrogen therapy. Causal inference for relies on strong temporal precedence (risk escalating with duration and dose) and biological plausibility via overexpression in meningioma tissues, though confounding by indication—such as MPA use in conditions like that may independently elevate baseline meningioma risk—cannot be fully excluded without randomized data. No similar dose-response patterns have emerged for or endometrial tumors in long-term follow-up, supporting differential tumor-specific effects.

HIV Acquisition Risk Debate

Observational studies and meta-analyses have suggested an association between depot medroxyprogesterone acetate (DMPA) use and increased acquisition risk in women, with relative risks estimated at 1.4 to 1.5 in some individual participant data analyses pooling data from multiple cohorts. 31288-7/fulltext) These findings, drawn primarily from non-randomized designs, indicate a potential 40-50% elevation in incidence compared to non-users or users of other methods, though residual from factors such as sexual behavior, partner status, and healthcare access complicates interpretation.31288-7/fulltext) Laboratory investigations, including a 2025 spatial transcriptomics study of cervical tissue, have identified DMPA-associated mucosal alterations such as upregulated immunoglobulin genes and immune markers potentially enhancing viral entry and , alongside prior models showing epithelial barrier impairment and increased target cell recruitment in the female genital tract. In contrast, randomized controlled trials (RCTs), considered higher-quality evidence, have not confirmed a significant risk increment. The 2019 ECHO trial, involving over 7,800 African women randomized to DMPA-IM, levonorgestrel implant, or copper intrauterine device, reported HIV incidence rates of 3.81, 3.29, and 3.31 per 100 woman-years respectively, with no statistically significant differences across arms despite high overall incidence.31288-7/fulltext) A 2025 Cochrane review synthesizing RCTs similarly concluded little to no difference in HIV acquisition for DMPA versus copper IUD (risk ratio 1.02, 95% CI 0.82-1.26), emphasizing that observational signals may reflect unmeasured confounders rather than causation. Causation remains unestablished, as no direct mechanistic pathway from DMPA to HIV susceptibility has been definitively proven in human RCTs, and some randomized mucosal endpoint studies show no adverse changes attributable to DMPA. DMPA's role in averting unintended may indirectly mitigate transmission risks, as pregnancy itself elevates maternal susceptibility through physiological and behavioral factors.31288-7/fulltext) Public health authorities, including the WHO and CDC, continue to endorse DMPA in high--prevalence settings where alternatives are limited, classifying it as a viable option without restriction based on HIV risk alone, given that discontinuing access could elevate rates and associated health burdens exceeding any unconfirmed HIV increment.

Ongoing Research and Future Directions

Current Studies

Recent longitudinal studies utilizing (DEXA) scans have confirmed partial bone mineral density (BMD) recovery following depot medroxyprogesterone acetate (DMPA) discontinuation, with rates varying by prior use duration; for instance, spine BMD recovers to baseline within approximately 30 months after short-term (<12 months) use, though full recovery may be incomplete after prolonged exposure. Investigations into meningioma mechanisms have identified progesterone receptor overexpression in affected tumors, particularly in models linking progestin exposure like MPA to tumor development; a 2025 analysis found all meningiomas in pregnant or postpartum cases—high-progestin states—expressed progesterone receptors, compared to 75.7% in non-pregnant controls, supporting causal hypotheses via receptor-mediated growth. Comparative trials of subcutaneous DMPA (Sayana Press, 104 mg) versus intramuscular Depo-Provera (150 mg) demonstrate equivalent contraceptive efficacy with stable pharmacokinetics, though self-administration yields higher continuation rates (up to 88% at 6 months) and minor skin irritation differences. Ongoing cohorts in HIV-endemic regions, building on prior trials like ECHO, continue evaluating DMPA's potential immunomodulatory effects on acquisition risk, with recent analyses showing no excess susceptibility in reproductive tract immune cells from DMPA users versus controls.

Potential New Applications

Medroxyprogesterone acetate (MPA) has been explored for palliation in advanced prostate cancer, leveraging its capacity to suppress testosterone levels and alleviate vasomotor symptoms associated with androgen deprivation therapy (ADT). A 2009 randomized trial demonstrated MPA's efficacy comparable to venlafaxine and cyproterone acetate in reducing hot flash frequency and severity in men undergoing ADT for prostate cancer, with MPA at 20 mg daily yielding significant symptom relief without substantial interference with ongoing hormonal treatments. Earlier historical applications included MPA as a secondary hormonal agent in hormone-refractory cases, where it contributed to temporary disease stabilization through progestogenic androgen suppression, though modern revival focuses on adjunctive symptom management amid resistance to primary therapies. In preclinical and small-scale human studies, MPA exhibits neuroprotective effects via positive modulation of specific GABAA receptor subtypes, potentially offering benefits for epilepsy and anxiety disorders. A 2022 in vitro analysis confirmed MPA's selective enhancement of alpha-2 and alpha-5 GABAA receptors—implicated in anxiolytic and anticonvulsant actions—without affecting alpha-1 subtypes linked to sedation. Pilot clinical evaluations from the 1980s in women with refractory epilepsy reported seizure frequency reductions of up to 50% following MPA addition to antiepileptic regimens at doses of 100-400 mg monthly, attributed to progesterone-like GABAergic potentiation, though larger controlled trials remain absent. High-dose MPA is under investigation for treating non-cancer cachexia and wasting syndromes, positioning it as an alternative to for appetite stimulation and weight preservation in conditions like chronic illness or geriatric frailty. A 2016 systematic review highlighted MPA's orexigenic effects in non-oncologic cachexia models, with doses of 500-1000 mg daily promoting lean mass retention via cytokine suppression, outperforming placebo in preliminary metabolic trials but requiring head-to-head comparisons with to assess thromboembolic risk differentials. Unlike cancer-specific applications, these efforts emphasize MPA's anti-inflammatory modulation of serotonin and tumor necrosis factor pathways to counter multifactorial wasting without neoplastic confounders. Emerging preclinical data suggest long-acting MPA formulations as adjuncts in HIV pre-exposure prophylaxis (PrEP) multipurpose technologies, hypothetically mitigating mucosal inflammation to enhance barrier integrity alongside antiretrovirals. A 2023 murine study integrated MPA with cabotegravir and dolutegravir in injectable depots, demonstrating sustained release without inducing local inflammation and preserving contraceptive efficacy, potentially addressing HIV acquisition vulnerabilities in high-risk populations despite observational links between depot MPA and elevated susceptibility. This approach remains hypothetical, as human trials must reconcile MPA's variable effects on genital tract immunity—sometimes downregulating epithelial genes akin to inflammatory states—with PrEP's protective overlay.

Mitigation of Known Risks

To mitigate bone mineral density (BMD) loss associated with depot medroxyprogesterone acetate (DMPA), guidelines recommend calcium supplementation (at least 1,300 mg daily) and vitamin D (600 IU daily), alongside weight-bearing exercise. Dual-energy X-ray absorptiometry (DXA) screening is advised for adolescents, long-term users (>2 years), or those with risk factors for , with discontinuation considered if other contraceptive options are suitable. Post-discontinuation, BMD recovery is typically substantial and reversible in adults, with annual gains of 0.3–2.0% depending on prior duration and site, though adolescents with >2 years of use may show incomplete hip recovery even after 5 years. For venous thromboembolism (VTE) risk, DMPA should be avoided (U.S. Medical Eligibility Criteria category 3) in women with or other high-risk conditions such as active VTE or certain inherited disorders. Short-term use is preferred when possible, with screening for personal or family history of prior to initiation to identify contraindications. Discontinuation is required if symptoms (e.g., leg swelling, ) emerge. Meningioma risk, linked to prolonged high-dose or injectable MPA exposure, can be reduced by limiting cumulative duration to less than 1 year where feasible and avoiding use in those with a history of (contraindicated). Patients should be monitored for neurological symptoms such as persistent headaches, vision changes, or seizures, with immediate discontinuation if is diagnosed, as tumor shrinkage has been observed post-cessation in some cases. To address potential acquisition risk, counseling on dual-method contraception—combining DMPA with consistent male condom use—is standard to reduce exposure. In high-prevalence settings, (PrEP) should be discussed and offered if indicated, with consideration of switching to non-DMPA methods (e.g., implant) for women at elevated risk per WHO category 2 guidance.

Veterinary Applications

Use in Animals

Medroxyprogesterone acetate (MPA) is employed in veterinary practice primarily to suppress estrus and prevent unwanted pregnancies in female dogs and cats. In dogs, subcutaneous or intramuscular injections of MPA, typically at doses of 2 to 5 mg/kg every 3 to 6 months, effectively inhibit ovarian activity and halt cycles, allowing deferral of breeding or spaying. Similar dosing regimens in cats achieve estrus suppression, often used off-label where no FDA-approved progestin exists specifically for this purpose, though it was previously labeled for such use before product withdrawal. Clinical trials and observational data indicate high efficacy in contraception, with MPA reducing estrous production and preventing conception in treated females when administered prior to or during proestrus; one early formulation achieved reliable suppression in bitches and , though exact rates vary by timing and dosage adherence. In male dogs and cats, MPA has been applied off-label for behavioral management, such as reducing mounting and linked to testosterone, via similar injectable protocols. In , MPA has been investigated for in captive and species, including delivery via for remote administration to large mammals like in overpopulated reserves, aiming to curb reproduction without . Field applications in southern African contexts have explored progestins like MPA for suppressing in and other ungulates, with trials demonstrating temporary contraception efficacy exceeding 90% in monitored groups when boosters are applied annually. However, adoption remains limited due to logistical challenges in free-ranging populations and the need for repeated dosing.

Efficacy and Safety in Veterinary Medicine

Medroxyprogesterone acetate (MPA) is employed in primarily for estrus suppression and contraception in companion animals such as dogs, cats, and ferrets, often administered via injection to manage reproductive behaviors and prevent unwanted litters. In dogs, MPA effectively postpones estrus when given subcutaneously at doses of 2-5 mg/kg, with studies demonstrating sustained suppression for several months, serving as a non-surgical option in cases of mismating or behavioral issues associated with heat cycles. Similarly, in cats, low-dose oral or injectable MPA (0.01-0.03 mg/kg daily) has shown promise in controlling reproduction, though long-term efficacy requires further validation to confirm ovulation blockade without rebound . Efficacy in ferrets includes suppression of prolonged estrus in jills, where MPA injections historically reduced ovarian activity comparably to other progestins, preventing mating and associated health risks like toxicity from unovulated follicles. In managed colonies, progestin treatments like MPA have achieved up to 90% reduction in litter rates when integrated into protocols, offering a reversible alternative to surgical sterilization for overpopulation in shelters or groups. However, deslorelin implants are increasingly preferred over MPA due to more consistent long-term suppression of and adrenal function without equivalent progestogenic side effects. Safety concerns with MPA in veterinary use are notable, particularly with repeated or high-dose administration, which can induce corticosteroid-like effects including adrenal suppression via inhibition of the hypothalamic-pituitary-adrenal axis. In dogs and cats, common adverse events encompass increased appetite, , , , , and elevated risk of diabetes mellitus, , and mammary tumors, with mammary adenocarcinomas reported in male cats following exposure. Ferrets exhibit species-specific issues such as coat color changes, hair thinning, and potential , prompting caution for prolonged use in this sensitive species where adrenal disease predisposition complicates outcomes. Long-term rodent studies have linked MPA to rare tumor induction, but these findings have limited translation to larger animals or clinical veterinary settings due to dosing disparities and species differences. Regulatory status reflects off-label application in many jurisdictions; while MPA (as Depo-Provera) is FDA-approved for use, veterinary administration in the U.S. typically occurs extra-label under veterinary oversight, with historical approval for growth promotion in withdrawn in the due to residue concerns in products, shifting focus to companion animal contraception. Guidelines from bodies like WSAVA emphasize monitoring for adverse effects and recommend alternatives like GnRH agonists for safer, more targeted reproductive control, underscoring MPA's role as a bridge therapy rather than first-line due to its side effect profile.

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