Sharp R B, Penning T M
Department of Pharmacology, University of Pennsylvania School of Medicine, Philadelphia 19104-6084.
Steroids. 1988 May-Jun;51(5-6):441-57. doi: 10.1016/0039-128x(88)90043-8.
The biosynthesis of progesterone from [3H]pregnenolone was curvilinear over a 6 h time course in human placenta cytotrophoblasts and in human placenta choriocarcinoma cells (JEG-3 cells). Mass measurements determined independently by radioimmunoassay indicate that the progesterone synthesized by cytotrophoblasts (21.0 +/- 5.20 ng/6 h/mg protein) is substantially higher than that synthesized by the JEG-3 cells (4.48 +/- 0.56 ng/6 h/mg protein). Two tight binding inhibitors of 3 beta-hydroxysteroid dehydrogenase (2 alpha-cyanoprogesterone I and cyanoketone II), and a potent inhibitor of the microsomal conversion of pregnenolone to progesterone (2 alpha-bromo-5 alpha-androstan-3-one-17 beta-acetate III) were compared as inhibitors of progesterone synthesis in the two cell-types. Compounds I and II were very potent inhibitors yielding IC50 values of between 10 and 20 nM. At higher concentrations (100 nM - 1,000 nM) compound I promoted a complete cessation of progesterone synthesis which could be reversed by washing the cells free of inhibitor. By contrast compound III was ineffectual as an inhibitor yielding an IC50 value greater than 10 microM. This 1,000-fold difference in inhibitory potency suggests that 2 alpha-cyano-substituted steroids display an unusual capacity to inhibit progesterone biosynthesis and secretion in normal and transformed human cells.
在人胎盘细胞滋养层细胞和人胎盘绒毛膜癌细胞(JEG - 3细胞)中,[3H]孕烯醇酮合成孕酮的过程在6小时的时间进程中呈曲线状。通过放射免疫测定法独立测定的质量测量结果表明,细胞滋养层细胞合成的孕酮(21.0±5.20 ng/6小时/毫克蛋白质)显著高于JEG - 3细胞合成的孕酮(4.48±0.56 ng/6小时/毫克蛋白质)。比较了3β - 羟基类固醇脱氢酶的两种紧密结合抑制剂(2α - 氰基孕酮I和氰基酮II)以及孕烯醇酮向孕酮微粒体转化的一种有效抑制剂(2α - 溴 - 5α - 雄甾 - 3 - 酮 - 17β - 乙酸酯III)作为两种细胞类型中孕酮合成抑制剂的效果。化合物I和II是非常有效的抑制剂,IC50值在10至20 nM之间。在较高浓度(100 nM - 1000 nM)下,化合物I可使孕酮合成完全停止,通过洗涤去除抑制剂后可逆转。相比之下,化合物III作为抑制剂无效,IC50值大于10 μM。这种抑制效力的1000倍差异表明,2α - 氰基取代的类固醇在正常和转化的人类细胞中具有抑制孕酮生物合成和分泌的异常能力。
