视黄酸诱导基因8(Stra8)的表达以及视黄酸在体外诱导小鼠生殖母细胞和精原细胞的成熟
Expression of stimulated by retinoic acid gene 8 (Stra8) and maturation of murine gonocytes and spermatogonia induced by retinoic acid in vitro.
作者信息
Zhou Qing, Li Ying, Nie Rong, Friel Patrick, Mitchell Debra, Evanoff Ryan M, Pouchnik Derek, Banasik Brent, McCarrey John R, Small Christopher, Griswold Michael D
机构信息
School of Molecular Biosciences, Washington State University, Pullman, WA 99164, USA.
出版信息
Biol Reprod. 2008 Mar;78(3):537-45. doi: 10.1095/biolreprod.107.064337. Epub 2007 Nov 21.
Vitamin A deficiency in the mouse results in an arrest in the progression of undifferentiated spermatogonia to differentiating spermatogonia. The supplement of retinol to vitamin-A-deficient mice reinitiates spermatogenesis in a synchronous manner throughout the testes. It is unclear whether the effects of retinoids are the result of a direct action on germ cells or are indirectly mediated through Sertoli cells. The expression of Stimulated by retinoic acid gene 8 (Stra8), which is required for spermatogenesis, is directly related to the availability of retinoic acid (RA). Analysis of gene expression by microarrays revealed moderate levels of Stra8 transcript in gonocytes and high levels in A and B spermatogonia. Stra8 mRNA levels were greatly reduced or absent in germ cells once they entered meiosis. This study examined the effect of retinoic acid on cultured neonatal testes and isolated gonocytes/spermatogonia in vitro. THY1(+) and KIT(+) germ cells were isolated by magnetic-activated cell sorting from the testes of mice of different ages. Isolated germ cells were cultured and treated with either vehicle (ethanol) or RA without feeder cells. We found that 1) Stra8 is predominantly expressed in premeiotic germ cells, 2) RA stimulates gonocyte DNA replication and differentiation in cultured neonatal testes, 3) in the absence of feeder cells, RA directly induces the transition of undifferentiated spermatogonia to differentiating spermatogonia by stimulating Stra8 and Kit gene expression, 4) RA dramatically stimulates Stra8 expression in undifferentiated spermatogonia but has a lesser impact in differentiating spermatogonia, 5) endogenous Stra8 gene expression is higher in differentiating spermatogonia than in undifferentiated spermatogonia and could mediate the RA effects on spermatogonial maturation, and 6) RA stimulates a group of genes involved in the metabolism, storage, transport, and signaling of retinoids.
小鼠体内维生素A缺乏会导致未分化精原细胞向分化型精原细胞的发育进程停滞。给维生素A缺乏的小鼠补充视黄醇可使整个睾丸同步重新启动精子发生。目前尚不清楚类视黄醇的作用是直接作用于生殖细胞的结果,还是通过支持细胞间接介导的。精子发生所需的视黄酸诱导基因8(Stra8)的表达与视黄酸(RA)的可利用性直接相关。通过微阵列分析基因表达发现,Stra8转录本在生殖母细胞中水平适中,在A和B型精原细胞中水平较高。一旦生殖细胞进入减数分裂,Stra8 mRNA水平会大幅降低或消失。本研究检测了视黄酸对体外培养的新生睾丸以及分离的生殖母细胞/精原细胞的影响。通过磁激活细胞分选从不同年龄小鼠的睾丸中分离出THY1(+)和KIT(+)生殖细胞。分离出的生殖细胞在无饲养细胞的情况下进行培养并用溶剂(乙醇)或RA处理。我们发现:1)Stra8主要在减数分裂前的生殖细胞中表达;2)RA可刺激体外培养的新生睾丸中生殖母细胞的DNA复制和分化;3)在无饲养细胞的情况下,RA通过刺激Stra8和Kit基因表达直接诱导未分化精原细胞向分化型精原细胞转变;4)RA显著刺激未分化精原细胞中Stra8的表达,但对分化型精原细胞的影响较小;5)分化型精原细胞中内源性Stra8基因表达高于未分化精原细胞,且可能介导RA对精原细胞成熟的作用;6)RA刺激一组参与类视黄醇代谢、储存、运输和信号传导的基因。
Zotero 插件