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C/EBPβ在雌性生殖中的重要作用。

An essential role for C/EBPbeta in female reproduction.

作者信息

Sterneck E, Tessarollo L, Johnson P F

机构信息

Advanced Bioscience Laboratories, Inc.-Basic Research Program, National Cancer Institute-Frederick Cancer Research and Development Center, Maryland 21702-1201, USA.

出版信息

Genes Dev. 1997 Sep 1;11(17):2153-62. doi: 10.1101/gad.11.17.2153.

Abstract

A large number of intercellular signaling molecules have been identified that orchestrate female reproductive physiology. However, with the exception of steroid hormone receptors, little information exists about the transcriptional regulators that mediate cellular responses to these signals. The transcription factor C/EBP beta (CCAAT/enhancer-binding protein beta) is expressed in ovaries and testes, as well as many other tissues of adult mice. Here we show that mice carrying a targeted deletion of the C/EBP beta gene exhibit reproductive defects. Although these animals develop normally and males are fertile, adult females are sterile. Transplantation of normal ovaries into mutant females restored fertility, thus localizing the primary reproductive defect to the ovary proper. In normal ovaries, C/EBP beta mRNA is specifically induced by luteinizing hormone (LH/hCG) in the granulosa layer of preovulatory antral follicles. C/EBP beta-deficient ovaries lack corpora lutea and fail to down-regulate expression of the prostaglandin endoperoxidase synthase 2 and P450 aromatase genes in response to gonadotropins. These findings demonstrate that C/EBP beta is essential for periovulatory granulosa cell differentiation in response to LH. C/EBP beta is thus established as a critical downstream target of G-protein-coupled LH receptor signaling and one of the first transcription factors, other than steroid hormone receptors, known to be required for ovarian follicle development in vivo.

摘要

大量细胞间信号分子已被鉴定出来,它们共同协调女性生殖生理过程。然而,除了类固醇激素受体外,关于介导细胞对这些信号作出反应的转录调节因子的信息却很少。转录因子C/EBPβ(CCAAT/增强子结合蛋白β)在成年小鼠的卵巢、睾丸以及许多其他组织中均有表达。在此我们表明,携带C/EBPβ基因靶向缺失的小鼠表现出生殖缺陷。尽管这些动物发育正常且雄性具有生育能力,但成年雌性是不育的。将正常卵巢移植到突变雌性小鼠体内可恢复生育能力,从而将主要生殖缺陷定位到卵巢本身。在正常卵巢中,促黄体生成素(LH/hCG)可在排卵前有腔卵泡的颗粒层中特异性诱导C/EBPβ mRNA的表达。缺乏C/EBPβ的卵巢没有黄体,并且在对促性腺激素作出反应时无法下调前列腺素内过氧化物合酶2和P450芳香化酶基因的表达。这些发现表明,C/EBPβ对于LH刺激下排卵前颗粒细胞的分化至关重要。因此,C/EBPβ被确立为G蛋白偶联的LH受体信号传导的关键下游靶点,也是已知的体内卵巢卵泡发育所需的除类固醇激素受体外的首批转录因子之一。

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An essential role for C/EBPbeta in female reproduction.C/EBPβ在雌性生殖中的重要作用。
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