孕酮通过 PGRMC1 调节的基因表达部分抑制细胞凋亡。
Progesterone inhibits apoptosis in part by PGRMC1-regulated gene expression.
机构信息
Department of Cell Biology, University of Connecticut Health Center, Farmington, CT 06030, USA.
出版信息
Mol Cell Endocrinol. 2010 May 14;320(1-2):153-61. doi: 10.1016/j.mce.2010.02.005. Epub 2010 Feb 6.
Abstract
Progesterone receptor membrane component-1 (PGRMC1) is present in both the cytoplasm and nucleus of spontaneously immortalized granulosa cells (SIGCs). PGRMC1 is detected as a monomer in the cytoplasm and a DTT-resistant PGRMC1 dimer in the nucleus. Transfected PGRMC1-GFP localizes mainly to the cytoplasm and does not form a DTT-resistant dimer. Moreover, forced expression of PGRMC1-GFP increases the sensitivity of the SIGCs to progesterone (P4)'s anti-apoptotic action, indicating that the PGRMC1 monomer is functional. However, when endogenous PGRMC1 is depleted by siRNA treatment and replaced with PGRMC1-GFP, P4 responsiveness is not enhanced, although overall levels of PGRMC1 are increased. P4's anti-apoptotic action is also attenuated by actinomycin D, an inhibitor of RNA synthesis, and P4 activation of PGRMC1 suppresses Bad and increases Bcl2a1d expression. Taken together, the present studies suggest a genomic component to PGRMC1's anti-apoptotic mechanism of action, which requires the presence of the PGRMC1 dimer.
摘要
孕激素受体膜组份 1(PGRMC1)存在于自发永生化颗粒细胞(SIGCs)的细胞质和细胞核中。在细胞质中检测到单体形式的 PGRMC1,而在细胞核中检测到二硫苏糖醇(DTT)抗性的 PGRMC1 二聚体。转染的 PGRMC1-GFP 主要定位于细胞质,不会形成 DTT 抗性二聚体。此外,强制表达 PGRMC1-GFP 增加了 SIGCs 对孕激素(P4)抗凋亡作用的敏感性,表明 PGRMC1 单体具有功能。然而,当通过 siRNA 处理耗尽内源性 PGRMC1 并用 PGRMC1-GFP 替代时,尽管总体 PGRMC1 水平增加,但 P4 的反应性并未增强。RNA 合成抑制剂放线菌素 D 也会削弱 P4 的抗凋亡作用,并且 P4 对 PGRMC1 的激活会抑制 Bad 并增加 Bcl2a1d 的表达。综上所述,本研究表明 PGRMC1 抗凋亡作用机制存在基因组成分,这需要 PGRMC1 二聚体的存在。
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