RU486 (MIFEPRISTONE): Mechanisms of Action and Clinical Uses

Cadepond, Françoise; Ulmann, André; Ee, Baulieu

doi:10.1146/annurev.med.48.1.129

Cited by 374 publications

(294 citation statements)

References 165 publications

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“…The steroid mifepristone is a remarkably active antiprogesterone and at high concentrations also an antagonist of GR action (Cadepond et al, 1997). The treatment of depression needs high dose of mifepristone, 600 or 1200 mg/ day.…”

Section: Discussionmentioning

confidence: 99%

“…With this procedure, the dose was swallowed completely and the stress caused to the animals was minimized, because control rats that received milk in the same way showed no stress-induced behavior change. Mifepristone is an antagonist of both progesterone receptor and GR (Cadepond et al, 1997). In the clinic, a low dose of 50 mg/ day mifepristone had an obvious antiprogesterone effect but no effects on cortisol, and only the high dose of 600 mg/day could antagonize GR (Belanoff et al, 2002).…”

Section: Pharmacological Treatmentmentioning

confidence: 99%

See 1 more Smart Citation

Mifepristone Repairs Region-Dependent Alteration of Synapsin I in Hippocampus in Rat Model of Depression

Han

Wang

et al. 2007

Neuropsychopharmacol

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Clinical investigations present much evidence that the glucocorticoid receptor (GR) antagonist mifepristone leads to a rapid amelioration of depression. The molecular mechanisms of mifepristone involved in the treatment of depression are not fully understood. Depression is associated with hippocampal plasticity, for which increased excitatory amino acid (EAA) release in CA3 induced by chronic stress is responsible, and glucocorticoids have a permissive role and act synergistically with EAAs in producing neuronal damage. Moreover, glucocorticoids increase synapsin I, which has a key role in the release of neurotransmitter, including EAAs. Hereby, we hypothesize that major depression involves synapsin I alteration and that mifepristone blocks this alteration. In the present study, we observed both the expression of hippocampal synapsin I and depression-associated behavior in a rat model of depression induced by chronic unpredictable mild stress (CUMS). The result showed that a region-dependent synapsin I alteration occurs in the rat hippocampus after 21 days of CUMS, that is, it increases in dentate gyrus (DG)/CA3 and decreases in the CA1 region. Correlation analysis indicated that the decrease of synapsin I in CA1 is highly correlated with the increase in the DG/CA3 subfield. Simultaneously, the region-dependent alteration of synapsin I is correlated with depression-associated behaviors. Both the alteration of synapsin I and the depression-associated behavior were rapidly restored after treatment with mifepristone for 1 week. The result suggests that the molecular mechanism underlying the treatment of depression with mifepristone is associated with the rapid repair of the synaptic alteration.

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Section: Discussionmentioning

confidence: 99%

Section: Pharmacological Treatmentmentioning

confidence: 99%

Mifepristone Repairs Region-Dependent Alteration of Synapsin I in Hippocampus in Rat Model of Depression

Han

Wang

et al. 2007

Neuropsychopharmacol

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“…Progesterone receptor blockers such as aglépristone (RU 46534) and mifepristone (RU 38486) are competitive antagonists of the progesterone receptor [14,15]. Aglépristone is the first progesterone receptor blocker licensed for veterinary use and has been used efficiently to terminate pregnancy [16,17] and to induce parturition [18].…”

Section: Introductionmentioning

confidence: 99%

Treatment of growth hormone excess in dogs with the progesterone receptor antagonist aglépristone

et al. 2006

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Acromegaly or hypersomatotropism in dogs is almost always due to progestin-induced hypersecretion of GH originating from the mammary gland. The aim of this study was to investigate whether aglépristone, a progesterone receptor antagonist, can be used to treat this form of canine acromegaly. In five Beagle bitches hypersomatotropism was induced by administration of MPA for over 1 year. Subsequently, aglépristone was administered. Blood samples were collected before MPA administration, immediately before, during, and 3.5 and 5.5 weeks after the last administration of aglépristone for determination of the plasma concentrations of GH and IGF-I. In addition, blood samples for the determination of the 6-h plasma profile of GH were collected before MPA administration, before aglépristone administration, and 1 week after the last aglépristone treatment.MPA administration resulted in a significant increase of the mean plasma IGF-I concentration, whereas analysis of the pulsatile plasma profile demonstrated a trend (P = 0.06) for a higher mean basal plasma GH concentration and a higher mean AUC 0 for GH. Treatment with aglépristone resulted in a significant decrease of the mean plasma GH and IGF-I concentrations. Analysis of the pulsatile plasma profile showed a trend (P = 0.06) for a lower mean basal plasma GH concentration and a lower mean AUC 0 for GH 1 week after the last aglépristone treatment compared with these values before aglépristone administration. Three and a half and 5.5 weeks after the last aglépristone administration the mean plasma IGF-I concentration increased again.In conclusion, aglépristone can be used successfully to treat dogs with progestin-induced hypersomatotropism. #

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“…These cells proved to be an excellent model for delineating the function of progesterone and its analogues. Progesterone was shown to induce remarkable growth inhibition and focal adhesion in the PR-transfected MDA-MB-231 cells ABC28 (Lin et al, 1999(Lin et al, , 2000.RU486 has proved to be a remarkable antiprogesterone and antiglucocorticoid agent in clinical applications since its birth some 20 years ago (Cadepond et al, 1997;Herrmann et al, 1982;Gaillard et al, 1983;Spitz and Chwalisz, 2000). In ABC28 cells, RU486 demonstrated mixed properties.…”

mentioning

confidence: 99%

“…There has been increasing interest in the development of antiprogestins for both anti-neoplastic and obstetrical applications (Cadepond et al, 1997;Gravanis et al, 1985;Rocereto et al, 2000). However, some of the progesterone antagonists can have undesired agonist-like effects that are associated with cell, tissue and species specificity.…”

mentioning

confidence: 99%

Demonstration of mixed properties of RU486 in progesterone receptor (PR)-transfected MDA-MB-231 cells: a model for studying the functions of progesterone analogues

Lin

et al. 2001

Br J Cancer

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Summary Progesterone antagonist RU486 (mifepristone) has been implicated for many anti-neoplastic and obstetrical applications. But the compound has demonstrated undesired agonist-like effect depending on cell, tissue and species studied. Using PR-transfected breast cancer cells MDA-MB-231, this report describes the similarities and differences between progesterone-and RU486-mediated effects on cell growth, cell differentiation and, at the molecular level, on the activation of p44/p42 MAP kinases (MAPK). Like progesterone, RU486 inhibited cells growth by arresting the cells in G0/G1 phase of the cell cycle. In contrast to progesterone that induced cell spreading, RU486 induced a multipolar, stellate morphology. RU486-treated cells showed no increase of stress fibers, nor was there any increase of focal adhesions as progesterone-treated cells did. Furthermore, despite of the fact that both compounds inhibited cell growth, RU486 significantly stimulated the activation of p44/p42 MAP kinases whereas progesterone markedly inhibited the activation. Nonetheless, the effects of RU486 were PR-mediated and RU486 was able to antagonize the effect of progesterone on cell growth and focal adhesion. In conclusion, RU486 can act not only as a progesterone antagonist, a progesterone agonist but also induced morphological and molecular changes that were distinct from progesterone-mediated effects in PR-transfected MDA-MB-231 cells. The non-progesterone-like effect of RU486 may be mediated through a pathway that is different from the progesterone-mediated pathway, or it is the result of a blockade of certain critical step(s) in the progesterone-mediated pathway. MATERIALS AND METHODS ChemicalsProgesterone was obtained from Sigma Chemical Co (St. Louis, MO USA). RU486 (mifepristone) and ZK98299 (onapristone) were from Siniwest Holdings, Inc. All tissue culture plastics and reagents were obtained from GIBCO BRL, Life Technologies, Inc. Cell cultureMDA-MB-231 cells were obtained from American Tissue Culture Collection (ATCC) in 1995 at passage 28. MDA-MB-231 cells were cloned using 96-well plates by plating 0.5 cell/well. Clone 2 (known as MDA-MB-231-CL2) was selected for transfection studies. All cells were routinely maintained in phenol-red containing Dulbecco's Modified Eagle Medium (DMEM) supplemented with 7.5% fetal calf serum (FCS), 2 mM glutamine and 40 mg/l gentamycin. TransfectionMDA-MB-231-CL2 cells were transfected with PR expression vectors hPR1 and hPR2 coding for PR isoform B and isoform A, respectively, in pSG5 plasmid (Kastner et al, 1990). Vector pBK-CMV (Stratagene) containing the neomycin-resistant gene was cotransfected with hPR1 and hPR2. Details of transfection were described previously (Lin et al, 1999). Cell growthCells (2 × 10 4 ) in their late exponential growth phase were seeded onto the 6-well plates in phenol red-free DMEM supplemented with 2 mM L-glutamine, 40 mg/l gentamycin and 5% dextran-coated charcoal (DCC)-treated FCS (Test Medium). Treatment of FCS with dextran-coated charcoal was to remove fro...

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RU486 (MIFEPRISTONE): Mechanisms of Action and Clinical Uses

Cited by 374 publications

References 165 publications

Mifepristone Repairs Region-Dependent Alteration of Synapsin I in Hippocampus in Rat Model of Depression

Mifepristone Repairs Region-Dependent Alteration of Synapsin I in Hippocampus in Rat Model of Depression

Treatment of growth hormone excess in dogs with the progesterone receptor antagonist aglépristone

Demonstration of mixed properties of RU486 in progesterone receptor (PR)-transfected MDA-MB-231 cells: a model for studying the functions of progesterone analogues

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