Physiology: Effects of intermittent antiprogestin RU486 combined with cyclic medroxyprogesterone acetate on folliculogenesis and ovulation

Kekkonen, Raimo; Croxatto, Horacio B.; Lähteenmäki, Pekka; Salvatierra, Ana María; Tuominen, Juhani

doi:10.1093/oxfordjournals.humrep.a135929

Cited by 14 publications

(2 citation statements)

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“…Although 12 treatment cycles showed luteal activity (progesterone >9 nmol/l), a clear rupture of a pre‐ovulatory follicle (>15 mm) was seen in only one treatment cycle. These findings suggest that good contraception may be achieved with this sequential regimen 33 …”

Section: Clinical Trialsmentioning

confidence: 74%

The Potential of Mifepristone (Ru486) as a Female Contraceptive Drug

Sarkar

2002

Int J Clinical Practice

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SUMMARYThis article reviews the development of mifepristone (RU486) as a female contraceptive drug. Mifepristone is an orally active compound with nearly 40% bioavailability after first pass effect. The steady plasma level of mifepristone ranges from 65 nmol/l with 1 mg/day to 1 μmol/l with 10 mg/day and reaches 2.5 μmol/l, 4.5 μmol/l and 5.4 μmol/l with mifepristone 50 mg, 100 mg and 200 mg daily, respectively, over the treatment period. Inhibition of ovulation may be achieved at serum mifepristone concentration of 232.7 nmol/l. Mifepristone appears to antagonise progesterone at the pituitary level to suppress gonadotropin and steroid hormone secretion rather than to act primarily on the hypothalamus to delay or inhibit ovulation. In fact, the endometrium is most sensitive to mifepristone. Low‐dose mifepristone impairs luteal phase endometrial development and receptivity by altering endometrial parakine, cytokine and enzyme activity. Thus, low‐dose mifepristone can significantly reduce the rate of conception without inhibiting ovulation. However, further research is needed to standardise the dose and dose‐schedule to achieve the desired efficacy of low‐dose mifepristone for routine clinical use with minimal or no side‐effects.

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Section: Clinical Trialsmentioning

confidence: 74%

The Potential of Mifepristone (Ru486) as a Female Contraceptive Drug

Sarkar

2002

Int J Clinical Practice

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“…Combining progestins and anti-progestins could allow for regular cycles while maintaining anovulation. However, simultaneous and sequential cyclic co-administration of a progestin with an anti-progestin abolishes the anti-ovulatory action of the anti-progestin or the progestin (Croxatto et al, 1989; Oral contraception and ovarian activity Kekkonen et al, 1995;Kekkonen and Lahteenmaki, 1996;Van Heusden et al, 2000) but generally improves bleeding patterns.…”

Section: Anti-progestinsmentioning

confidence: 99%

Residual ovarian activity during oral steroid contraception

Heusden¹

2002

Human Reproduction Update

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Steroid drugs with contraceptive properties have been available in the clinical setting for over four decades and are still subject to improvement. Estrogens, progestins and anti-progestins have been used alone or in various combinations, regimens and routes of administration to favour the balance between efficacy and undesirable effects. One of the most important changes in this respect is the gradual lowering of steroid dosage in commercially available contraceptives. Current steroid contraceptive pills still achieve the goal of suppression of pituitary-ovarian activity, but the margins for error are minimal. In this review the available data on modes of action and the effects on suppressing pituitary-ovarian activity by different forms of oral contraception are reassessed. Although pregnancy rates provide a crude measure of contraceptive efficacy, no benchmark for pituitary-ovarian inhibition is available to test the suppressive potential of contraceptive drugs. Consequently, many studies provide incomplete and/or incomparable results. For the further study of those forms of steroid contraception that rely predominantly on suppression of ovarian activity, prevention of dominant follicles selection should be the objective.

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