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孕激素受体亚型在人子宫内膜基质细胞中的选择性及拮抗作用

Selective and opposing actions of progesterone receptor isoforms in human endometrial stromal cells.

作者信息

Yudt M R, Berrodin T J, Jelinsky S A, Hanna L A, Brown E L, Chippari S, Bhat R A, Winneker R C, Zhang Z

机构信息

Women's Health Research Institute, Wyeth Research, Collegeville, PA 19426, USA.

出版信息

Mol Cell Endocrinol. 2006 Mar 9;247(1-2):116-26. doi: 10.1016/j.mce.2005.12.012. Epub 2006 Jan 25.

DOI:10.1016/j.mce.2005.12.012
PMID:16442706
Abstract

Transcriptional regulation by progesterone is mediated primarily through the two progesterone receptor (PR) isoforms, PR-A and PR-B. Primary human endometrial stromal cell cultures, in which endogenous PR expression was lost, were infected with adenovirus expressing PR-A, PR-B, or both. Global gene expression analysis was conducted on vehicle and 30 nM progesterone (P4) treated cells following 12 h treatment. Interestingly, many genes regulated by PR-B alone or upon PR-A and PR-B co-expression, did not overlap with each other or with the PR-A expression group. Although many genes known to be progestin regulated in the uterus in vivo were also regulated in this study, markedly little overlap with published P4 regulated genes from human breast cancer cells was observed. Progesterone dose response curves were generated for several genes demonstrating gene selective potency and efficacy for each PR isoform. Furthermore, the PR isoforms opposed each other in regulation of tissue factor, with PR-B increasing and PR-A decreasing both mRNA and protein levels. Our data provide a view of global gene expression by PR isoforms in human endometrial cells and a comparison with other cell types. The specific genes and regulation patterns found provide groundwork to revealing the mechanism of PR isoform selectivity, and perhaps ultimately to the tissue selective properties these receptors appear to exhibit.

摘要

孕酮的转录调控主要通过两种孕酮受体(PR)亚型PR-A和PR-B介导。在原发性人子宫内膜基质细胞培养物中,内源性PR表达缺失,用表达PR-A、PR-B或两者的腺病毒进行感染。在12小时处理后,对用载体处理和用30 nM孕酮(P4)处理的细胞进行全局基因表达分析。有趣的是,许多仅由PR-B调控或由PR-A和PR-B共表达调控的基因,彼此之间以及与PR-A表达组均无重叠。尽管本研究中也调控了许多已知在体内子宫中受孕激素调控的基因,但与已发表的来自人乳腺癌细胞的P4调控基因的重叠明显较少。针对几个基因生成了孕酮剂量反应曲线,证明了每个PR亚型的基因选择性效力和功效。此外,PR亚型在组织因子的调控中相互拮抗,PR-B增加而PR-A降低mRNA和蛋白质水平。我们的数据提供了人子宫内膜细胞中PR亚型的全局基因表达情况,并与其他细胞类型进行了比较。所发现的特定基因和调控模式为揭示PR亚型选择性机制奠定了基础,也许最终能揭示这些受体似乎表现出的组织选择性特性。

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