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Xenotransplantation exposes the etiology of azoospermia factor (AZF) induced male sterility

机译:异种移植暴露了无精症因子(AZF)引起的男性不育的病因

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摘要

Ramathal et al. have employed an elegant xenotransplantation technique to study the fate of human induced pluripotent stem cells (hiPSCs) from fertile males and from males carrying Y chromosome deletions of the azoospermia factor (AZF) region. When placed in a mouse testis niche, hiPSCs from fertile males differentiate into germ cell-like cells (GCLCs). Highlighting the crucial role of cell autonomous factors in male sterility, hiPSCs derived from azoospermic males prove to be less successful under similar circumstances. Their studies argue that the agametic Sertoli cell only phenotype of two of the AZF deletions likely arises from a defect in the maintenance of germline stem cells (GSCs) rather than from a defect in their specification. These observations underscore the importance of the dialogue between the somatic niche and its inhabitant stem cells, and open up interesting questions concerning the functioning of the somatic niche and how it communicates to the GSCs.
机译:Ramathal等。已经采用了一种优雅的异种移植技术来研究人类诱导的多能干细胞(hiPSC)的命运,这些多能干细胞来自可育的雄性和携带无精子因子(AZF)区Y染色体缺失的雄性。当置于小鼠睾丸壁iche中时,来自可育雄性的hiPSC分化为生殖细胞样细胞(GCLC)。强调细胞自主因子在雄性不育中的关键作用,无精子雄性衍生的hiPSC在类似情况下被证明不太成功。他们的研究认为,两个AZF缺失的非配体性支持细胞仅表型可能是由于种系干细胞(GSC)的维持缺陷而不是其规格缺陷引起的。这些观察结果强调了体位生态位及其居民干细胞之间对话的重要性,并提出了有关体位生态位的功能及其如何与GSC交流的有趣问题。

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