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胰岛素样 3 信号对于睾丸下降很重要,但对于成年小鼠的精子发生和精原细胞存活是可有可无的。

Insulin-like 3 signaling is important for testicular descent but dispensable for spermatogenesis and germ cell survival in adult mice.

机构信息

Department of Human and Molecular Genetics, Herbert Wertheim College of Medicine, Florida International University, Miami, Florida 33199, USA.

出版信息

Biol Reprod. 2012 Dec 21;87(6):143. doi: 10.1095/biolreprod.112.103382. Print 2012 Jun.

Abstract

Relaxin family peptide receptor 2 (RXFP2) is the cognate receptor of a peptide hormone insulin-like 3 (INSL3). INSL3 is expressed at high levels in both fetal and adult Leydig cells. Deletion of Insl3 or Rxfp2 genes in mice caused cryptorchidism resulting from a failure of gubernaculum development. Using a novel mouse transgenic line with a knock-in LacZ reporter in the Rxfp2 locus, we detected a robust Rxfp2 expression in embryonic and early postnatal gubernaculum in males and in postmeiotic spermatogenic cells in adult testis. To study the role of INSL3/RXFP2 signaling in male reproduction, we produced a floxed Rxfp2 allele and used the Cre/loxP approach to delete Rxfp2 in different tissues. Using Cre transgene driven by retinoic acid receptor beta promoter, conditional gene targeting in gubernacular mesenchymal cells at early embryonic stages caused high intraabdominal cryptorchidism as in males with a global deletion of Rxfp2. However, when the Rxfp2 was deleted in gubernacular smooth or striated muscle cells, no abnormalities of testicular descent or testis development were found. Specific ablation of Rxfp2 in male germ cells using Stra8-icre transgene did not affect testis descent, spermatogenesis, or fertility in adult males. No significant change in germ cell apoptosis was detected in mutant males. In summary, our data indicate that the INSL3/RXFP2 signaling is important for testicular descent but dispensable for spermatogenesis and fertility in adult males.

摘要

松弛素家族肽受体 2 (RXFP2) 是一种肽激素胰岛素样 3 (INSL3) 的同源受体。INSL3 在胎儿和成人生殖嵴细胞中均高表达。在小鼠中敲除 Insl3 或 Rxfp2 基因会导致隐睾,这是由于生殖嵴发育失败所致。利用一种新型的小鼠转基因系,其 Rxfp2 基因座中带有一个敲入 LacZ 报告基因,我们在雄性胚胎和早期新生的生殖嵴以及成年睾丸的减数分裂后精子发生细胞中检测到强烈的 Rxfp2 表达。为了研究 INSL3/RXFP2 信号在雄性生殖中的作用,我们产生了一个 floxed Rxfp2 等位基因,并利用 Cre/loxP 方法在不同组织中删除 Rxfp2。使用视黄酸受体β启动子驱动的 Cre 转基因,在早期胚胎阶段对生殖嵴间质细胞进行条件性基因靶向,导致与 Rxfp2 全局缺失的雄性一样出现高腹腔内隐睾。然而,当生殖嵴平滑肌或横纹肌细胞中删除 Rxfp2 时,未发现睾丸下降或睾丸发育异常。使用 Stra8-icre 转基因特异性消融雄性生殖细胞中的 Rxfp2 不会影响成年雄性的睾丸下降、精子发生或生育能力。在突变雄性中未检测到精母细胞凋亡的显著变化。总之,我们的数据表明,INSL3/RXFP2 信号对睾丸下降很重要,但对成年雄性的精子发生和生育能力是可有可无的。

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