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首页> 外文期刊>Biology of Reproduction: Offical Journal of the Society for the Study of Reproduction >Identification of glial cell line-derived neurotrophic factor-regulated genes important for spermatogonial stem cell self-renewal in the rat.
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Identification of glial cell line-derived neurotrophic factor-regulated genes important for spermatogonial stem cell self-renewal in the rat.

机译:鉴定对大鼠精原干细胞自我更新重要的神经胶质细胞系神经营养因子调节基因。

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Spermatogonial stem cells (SSCs) provide the foundation for spermatogenesis throughout the life of a male. Because SSCs of many species can colonize the mouse testis, and glial cell line-derived neurotrophic factor (GDNF) is responsible for stimulating SSC self-renewal in rodents, we reasoned that molecular mechanisms of SSC self-renewal are similar across species. GDNF-regulated genes have been identified in mouse SSCs; however, downstream targets of GDNF are unknown in other species. The objective of this work was to identify GDNF-regulated genes in rat SSCs and to define the biological significance of these genes for rat SSC self-renewal. We conducted microarray analysis on cultured rat germ cells enriched for SSCs in the presence and absence of GDNF. Many GDNF-regulated genes were identified, most notably, Bcl6b and Etv5, which are important for mouse SSC self-renewal. Bcl6b was the most highly regulated gene in both the rat and mouse. Additionally, we identified three novel GDNF-regulated genes in rat SSCs: Bhlhe40, Hoxc4, and Tec. Small interfering RNA treatment for Bcl6b, Etv5, Bhlhe40, Hoxc4, and Tec resulted in a decrease in SSC number, as determined by transplantation, without a change in total cell number within the culture. These data indicate that, like in the mouse SSC, Bcl6b and Etv5 are important for rat SSC self-renewal, suggesting that these genes may be important for SSCs in all mammals. Furthermore, identification of three novel GDNF-regulated genes in the rat SSC extends our knowledge of SSC activity and broadens the foundation for understanding this process in higher species, including humans.
机译:精原干细胞(SSC)为男性一生中的精子发生奠定了基础。由于许多物种的SSC可以在小鼠睾丸中定居,而胶质细胞系衍生的神经营养因子(GDNF)则可以刺激啮齿动物的SSC自我更新,因此我们认为SSC自我更新的分子机制在各个物种之间都相似。已经在小鼠SSC中鉴定了GDNF调节的基因。但是,GDNF的下游靶标在其他物种中是未知的。这项工作的目的是鉴定大鼠SSC中GDNF调控的基因,并定义这些基因对大鼠SSC自我更新的生物学意义。在有和没有GDNF的情况下,我们对富含SSC的培养大鼠生殖细胞进行了微阵列分析。确定了许多GDNF调控的基因,最著名的是Bcl6b和Etv5,它们对小鼠SSC自我更新很重要。 Bcl6b是在大鼠和小鼠中被高度调控的基因。此外,我们在大鼠SSC中鉴定了三个新的GDNF调控基因:Bhlhe40,Hoxc4和Tec。对Bcl6b,Etv5,Bhlhe40,Hoxc4和Tec的小干扰RNA处理导致SSC数量减少(通过移植确定),而培养物中的总细胞数没有变化。这些数据表明,像在小鼠SSC中一样,Bcl6b和Etv5对大鼠SSC自我更新很重要,表明这些基因对于所有哺乳动物中的SSC都可能重要。此外,在大鼠SSC中鉴定三个新的GDNF调控基因扩展了我们对SSC活性的认识,并拓宽了在包括人类在内的更高物种中理解这一过程的基础。

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