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无翅型(WNT)信号通路是大鼠子宫基质细胞增殖的孕激素作用靶点。

WINGLESS (WNT) signaling is a progesterone target for rat uterine stromal cell proliferation.

作者信息

Rider Virginia, Talbott Alex, Bhusri Anuradha, Krumsick Zach, Foster Sierra, Wormington Joshua, Kimler Bruce F

机构信息

Department of BiologyPittsburg State University, Pittsburg, Kansas, USA

Department of BiologyPittsburg State University, Pittsburg, Kansas, USA.

出版信息

J Endocrinol. 2016 May;229(2):197-207. doi: 10.1530/JOE-15-0523. Epub 2016 Mar 14.

Abstract

Preparation of mammalian uterus for embryo implantation requires a precise sequence of cell proliferation. In rodent uterus, estradiol stimulates proliferation of epithelial cells. Progesterone operates as a molecular switch and redirects proliferation to the stroma by down-regulating glycogen synthase kinase-3β (GSK-3β) and stimulating β-catenin accumulation in the periluminal stromal cells. In this study, the WNT signal involved in the progesterone-dependent proliferative switch was investigated. Transcripts of four candidate Wnt genes were measured in the uteri from ovariectomized (OVX) rats, progesterone-pretreated (3 days of progesterone, 2mg/daily) rats, and progesterone-pretreated rats given a single dose (0.2µg) of estradiol. The spatial distribution of the WNT proteins was determined in the uteri after the same treatments. Wnt5a increased in response to progesterone and the protein emerged in the periluminal stromal cells of progesterone-pretreated rat uteri. To investigate whether WNT5A was required for proliferation, uterine stromal cell lines were stimulated with progesterone (1µM) and fibroblast growth factor (FGF, 50ng/mL). Proliferating stromal cells expressed a two-fold increase in WNT5A protein at 12h post stimulation. Stimulated stromal cells were cultured with actinomycin D (25µg/mL) to inhibit new RNA synthesis. Relative Wnt5a expression increased at 4 and 6 h of culture, suggesting that progesterone plus FGF preferentially increased Wnt5a mRNA stability. Knockdown of Wnt5a in uterine stromal cell lines inhibited stromal cell proliferation and decreased Wnt5a mRNA. The results indicate that progesterone initiates and synchronizes uterine stromal cell proliferation by increasing WNT5A expression and signaling.

摘要

哺乳动物子宫为胚胎着床做准备需要精确的细胞增殖序列。在啮齿动物子宫中,雌二醇刺激上皮细胞增殖。孕酮作为分子开关,通过下调糖原合酶激酶-3β(GSK-3β)并刺激β-连环蛋白在周缘基质细胞中积累,将增殖导向基质。在本研究中,对参与孕酮依赖性增殖转换的WNT信号进行了研究。在去卵巢(OVX)大鼠、经孕酮预处理(孕酮,2mg/天,共3天)的大鼠以及经孕酮预处理后给予单剂量(0.2µg)雌二醇的大鼠的子宫中,测量了四个候选Wnt基因的转录本。在相同处理后的子宫中确定了WNT蛋白的空间分布。Wnt5a对孕酮有反应而增加,且该蛋白出现在经孕酮预处理的大鼠子宫周缘基质细胞中。为了研究WNT5A是否是增殖所必需的,用孕酮(1µM)和成纤维细胞生长因子(FGF,50ng/mL)刺激子宫基质细胞系。刺激后12小时,增殖的基质细胞中WNT5A蛋白表达增加了两倍。用放线菌素D(25µg/mL)培养受刺激的基质细胞以抑制新的RNA合成。培养4小时和6小时时,Wnt5a相对表达增加,表明孕酮加FGF优先增加Wnt5a mRNA稳定性。子宫基质细胞系中Wnt5a的敲低抑制了基质细胞增殖并降低了Wnt5a mRNA。结果表明,孕酮通过增加WNT5A表达和信号传导来启动和同步子宫基质细胞增殖。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/458e/5064766/92c23239165f/joe-229-197-g001.jpg

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