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A human DAZ transgene confers partial rescue of the mouse Dazl null phenotype

机译:人类DAZ转基因可部分拯救小鼠Dazl无效表型

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摘要

In a subset of infertile men, a spectrum of spermatogenic defects ranging from a complete absence of germ cells (sertoli cell only) to oligozoospermia is associated with microdeletions of the DAZ (deleted in azoospermia) gene cluster on human distal Yq. DAZ encodes a testis-specific protein with RNA-binding potential recently derived from a single-copy gene DAZL1 (DAZ-like) on chromosome 3. Y chromosomal DAZ homologues are confined to humans and higher primates. It remains unclear which function unique to higher primate spermatogenesis DAZ may serve, and the functional status of the gene recently has been questioned. To assess the extent of functional conservation we have tested the capacity of a human DAZ gene contained in a 225-kb yeast artificial chromosome to complement the sterile phenotype of the Dazl null mouse (Dazl−/−), which is characterized by severe germ-cell depletion and meiotic failure. Although Dazl−/− mice remained infertile when the DAZ transgene was introduced, histological examination revealed a partial and variable rescue of the mutant phenotype, manifest as a pronounced increase in the germ cell population of the seminiferous tubules and survival to the pachytene stage of meiosis. As well as constituting definitive proof of the spermatogenic role of the DAZ gene product, these findings confirm the high degree of functional conservation between the DAZ and DAZL1 genes, suggesting they may constitute a single target for contraceptive intervention and raising the possibility of therapeutic up-regulation of the DAZL1 gene in infertile men.
机译:在部分不育男性中,从完全不存在生殖细胞(仅睾丸脂细胞)到少精子症的一系列生精缺陷与人类远端Yq上DAZ的微缺失(无精子症缺失)有关。 DAZ编码一种具有RNA结合潜能的睾丸特异性蛋白质,该蛋白质最近来自3号染色体上的单拷贝基因DAZL1(类DAZ)。Y染色体DAZ同源物仅限于人类和高等灵长类动物。尚不清楚哪种功能可以发挥更高的灵长类动物精子生成DAZ的功能,最近对该基因的功能状态提出了质疑。为了评估功能保守性的程度,我们测试了225kb酵母人工染色体中包含的人类DAZ基因补充Dazl无效小鼠(Dazl-/-)的无菌表型的能力,该表型的特征是严重的细菌-细胞耗竭和减数分裂衰竭。尽管当引入DAZ转基因时Dazl //-小鼠仍然不育,但是组织学检查显示突变表型的部分和可变拯救,表现为生精小管生殖细胞群的显着增加和减数分裂的上皮阶段的存活。这些发现不仅构成了DAZ基因产物生精作用的权威证据,还证实了DAZ和DAZL1基因之间高度的功能保守性,表明它们可能构成避孕措施的单一目标,并增加了治疗上的可能性。不育男性中DAZL1基因的调控。

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