In vitro and in vivo characterization of a novel nonsteroidal, species-specific progesterone receptor modulator, PRA-910.

Z Zhang, S G Lundeen, O Slayden, Y Zhu, J Cohen, T J Berrodin, J Bretz, S Chippari, J Wrobel, P Zhang, A Fensome, R C Winneker, M R Yudt
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Abstract

The progesterone receptor (PR) is an important regulator of female reproduction. Consequently, PR modulators have found numerous pharmaceutical utilities in women's reproductive health. In the process of identifying more receptor-specific and tissue-selective PR modulators, we discovered a novel nonsteroidal, 6-aryl benzoxazinone compound, PRA-910, that displays unique in vitro and in vivo activities. In a PR/PRE reporter assay in COS-7 cells, PRA-910 shows potent PR antagonist activity with an IC50 value of approximately 20 nM. In the alkaline phosphatase assay in the human breast cancer cell line T47D, PRA-910 is a partial progesterone antagonist at low concentrations and is also an effective PR agonist at higher concentrations (EC50 value of approximately 700 nM). PRA-910 binds to the human PR with high affinity (Kd = 4 nM) and was previously shown to exhibit greater than 100-fold selectivity for the PR versus other steroid receptors. In the adult ovariectomized rat, PRA-910 is a potent PR antagonist. It inhibits progesterone-induced uterine decidual response with an ED50 value of 0.4 mg/kg, p.o., and reverses progesterone suppression of estradiol-induced complement C3 expression with potency similar to RU-486. In the nonhuman primate, however, PRA-910 is a PR agonist. The effect on endometrial histology strongly resembles that of progesterone. This unique compound also suppresses estradiol-induced epithelial cell proliferation and both estrogen and progesterone receptor expression in the uterine endometrium as a PR agonist would. In summary, PRA-910 is a structurally and biologically novel selective PR modulator with either PR agonist or antagonist activity, depending on context, concentration, and species.

一种新型非甾体、物种特异性黄体酮受体调节剂PRA-910的体外和体内表征。
孕激素受体(PR)是女性生殖的重要调节因子。因此,PR调节剂在妇女生殖健康方面发现了许多医药用途。在鉴定更多受体特异性和组织选择性PR调节剂的过程中,我们发现了一种新的非甾体,6-芳基苯并杂嗪酮化合物PRA-910,它在体外和体内都具有独特的活性。在COS-7细胞的PR/PRE报告细胞实验中,PRA-910显示出有效的PR拮抗剂活性,IC50值约为20 nM。在人乳腺癌细胞系T47D的碱性磷酸酶试验中,PRA-910在低浓度下是部分黄体酮拮抗剂,在高浓度下也是有效的PR激动剂(EC50值约为700 nM)。PRA-910与人类PR具有高亲和力(Kd = 4 nM),并且先前显示对PR的选择性比其他类固醇受体高100倍。在切除卵巢的成年大鼠中,PRA-910是一种有效的PR拮抗剂。抑制黄体酮诱导的子宫蜕膜反应,ED50值为0.4 mg/kg, p.o,逆转黄体酮对雌二醇诱导的补体C3表达的抑制作用,其效价与RU-486相似。然而,在非人灵长类动物中,PRA-910是一种PR激动剂。对子宫内膜组织学的影响与黄体酮非常相似。这种独特的化合物还可以抑制雌二醇诱导的上皮细胞增殖以及子宫内膜中雌激素和孕激素受体的表达,就像PR激动剂一样。总之,PRA-910是一种结构和生物学上新颖的选择性PR调节剂,根据环境、浓度和物种的不同,具有PR激动剂或拮抗剂活性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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