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20α-羟基类固醇脱氢酶基因靶向敲除小鼠的生殖表型

Reproductive phenotypes in mice with targeted disruption of the 20alpha-hydroxysteroid dehydrogenase gene.

作者信息

Ishida Maho, Choi Jae-hyek, Hirabayashi Keiji, Matsuwaki Takashi, Suzuki Masatoshi, Yamanouchi Keitaro, Horai Reiko, Sudo Katsuko, Iwakura Yoichiro, Nishihara Masugi

机构信息

Department of Physiology, Interdisciplinary Graduate School of Medicine and Engineering, University of Yamanashi, Japan.

出版信息

J Reprod Dev. 2007 Jun;53(3):499-508. doi: 10.1262/jrd.18125. Epub 2007 Feb 2.

Abstract

In the corpus luteum of rats and mice, 20alpha-hydroxysteroid dehydrogenase (20alpha-HSD) catalyzes the conversion of progesterone to a biologically inactive metabolite, 20alpha-dihydroprogesterone (20alpha-OHP). The reduction of progesterone by 20alpha-HSD is believed to be important for functional luteolysis in these rodent species. In addition to the corpus luteum, expression of 20alpha-HSD has been demonstrated in tissues such as the placenta, endometrial epithelia, and fetal skin, although the roles it plays in the latter tissues remain to be determined. To determine the contribution of 20alpha-HSD to functional luteolysis and to the rodent reproductive system more generally, we generated a strain of mice with targeted disruption of the 20alpha-HSD gene. In the 20alpha-HSD-/- mice we obtained, which lacked the genomic region essential for catalytic reaction, neither 20alpha-HSD activity in the corpus luteum nor an increase in the serum concentrations of 20alpha-OHP during pseudopregnancy or pregnancy was detected. The durations of the estrous cycle, pseudopregnancy, and pregnancy were significantly prolonged in the 20alpha-HSD-/- mice, although the serum progesterone levels decreased to levels low enough for delivery of pups at term of pregnancy. In addition, the number of pups, especially live pups, was markedly decreased in the 20alpha-HSD-/- mice. These findings suggest that the role of 20alpha-HSD in functional luteolysis is relatively minor but that it is involved in the survival of newborn mice.

摘要

在大鼠和小鼠的黄体中,20α-羟类固醇脱氢酶(20α-HSD)催化孕酮转化为生物活性较低的代谢产物20α-二氢孕酮(20α-OHP)。20α-HSD介导的孕酮还原被认为对这些啮齿动物的功能性黄体溶解很重要。除黄体之外,在胎盘、子宫内膜上皮和胎儿皮肤等组织中也已证实有20α-HSD的表达,不过其在这些组织中所起的作用仍有待确定。为了更全面地确定20α-HSD对功能性黄体溶解及啮齿动物生殖系统的作用,我们培育出了一种20α-HSD基因靶向敲除的小鼠品系。在我们获得的20α-HSD-/-小鼠中,由于缺乏催化反应所必需的基因组区域,未检测到黄体中的20α-HSD活性,也未检测到假孕或妊娠期间血清中20α-OHP的升高。虽然妊娠足月时血清孕酮水平降至足以分娩幼崽的低水平,但20α-HSD-/-小鼠的动情周期、假孕和妊娠持续时间显著延长。此外,20α-HSD-/-小鼠的幼崽数量,尤其是存活幼崽的数量明显减少。这些发现表明,20α-HSD在功能性黄体溶解中的作用相对较小,但它与新生小鼠的存活有关。

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