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Geminin deletion in pre-meiotic DNA replication stage causes spermatogenesis defect and infertility

机译:减数分裂前DNA复制阶段的胚芽蛋白缺失导致精子发生缺陷和不育

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Geminin plays a critical role in cell cycle regulation by regulating DNA replication and serves as a transcriptional molecular switch that directs cell fate decisions. Spermatogonia lacking Geminin disappear during the initial wave of mitotic proliferation, while geminin is not required for meiotic progression of spermatocytes. It is unclear whether geminin plays a role in pre-meiotic DNA replication in later-stage spermatogonia and their subsequent differentiation. Here, we selectively disrupted Geminin in the male germline using the Stra8-Cre / loxP conditional knockout system. Geminin -deficient mice showed atrophic testes and infertility, concomitant with impaired spermatogenesis and reduced sperm motility. The number of undifferentiated spermatogonia and spermatocytes was significantly reduced; the pachytene stage was impaired most severely. Expression of cell proliferation-associated genes was reduced in Gmnnfl/Δ ; Stra8-Cre testes compared to in controls. Increased DNA damage, decreased Cdt1, and increased phosphorylation of Chk1/Chk2 were observed in Geminin -deficient germ cells. These results suggest that geminin plays important roles in pre-meiotic DNA replication and subsequent spermatogenesis.
机译:胚芽素通过调节DNA复制在细胞周期调控中发挥关键作用,并作为指导细胞命运决定的转录分子开关。缺乏Geminin的精原细胞在有丝分裂增殖的最初阶段消失,而对于精母细胞减数分裂进程则不需要geminin。尚不清楚geminin是否在晚期精原细胞的减数分裂前DNA复制及其随后的分化中发挥作用。在这里,我们使用Stra8-Cre / loxP条件敲除系统选择性地破坏了雄性种系中的Geminin。缺乏胚芽蛋白的小鼠表现出萎缩性睾丸和不育症,伴有精子发生受损和精子活动力降低。未分化的精原细胞和精母细胞数量明显减少;粗线期受损最严重。细胞增殖相关基因在Gmnn fl /Δ中的表达减少;与对照相比,Stra8-Cre睾丸比较。在缺乏Geminin的生殖细胞中观察到DNA损伤增加,Cdt1减少和Chk1 / Chk2磷酸化增加。这些结果表明,geminin在减数分裂前的DNA复制和随后的精子发生中起重要作用。

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