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首页> 外文期刊>Reproductive toxicology >HSV type 1 thymidine kinase protein accumulation in round spermatids induces male infertility by spermatogenesis disruption and apoptotic loss of germ cells.
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HSV type 1 thymidine kinase protein accumulation in round spermatids induces male infertility by spermatogenesis disruption and apoptotic loss of germ cells.

机译:HSV 1型胸苷激酶蛋白在圆形精子细胞中的积累通过精子发生破坏和生殖细胞凋亡而诱导男性不育。

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摘要

HSV type 1 thymidine kinase (HSV1-TK)-introduced transgenic rodents and HSV-infected humans were reported to suffer male infertility. The present study aimed to find novel clues to clarify the cause of HSV1-TK-induced male infertility using an HSV1-tk transgenic rat line. Two truncated HSV1-TK proteins, 37 and 39kDa, were produced and accumulated in the round spermatids, and their transcription initiation site was identified for the first time at the 65 base downstream of the translation start point of the full-length 43kDa HSV1-TK. Spermatozoa from those young transgenic rats showed malformed heads, looped tails, and missing cell membrane in heads and tails. Furthermore, age-dependent germ cell loss was observed. TUNEL assay suggested that this germ cell loss is caused by increased apoptotic germ cell death. These results suggest that the expression of HSV1-TK in testes brings about not only abnormal spermiogenesis but also a loss of germ cells due to apoptosis. These findings could provide a novel clue to elucidate the molecular mechanism underlying male infertility in transgenic animals and HSV-infected patients.
机译:据报道,由HSV 1型胸苷激酶(HSV1-TK)引入的转基因啮齿动物和被HSV感染的人类患有男性不育症。本研究旨在寻找新的线索,以阐明使用HSV1-tk转基因大鼠品系HSV1-TK诱导的男性不育的原因。在圆形的精子细胞中产生并积累了两个截短的HSV1-TK蛋白37和39kDa,它们的转录起始位点首次在全长43kDa HSV1-TK的翻译起点下游65个碱基处鉴定。这些年轻的转基因大鼠的精子表现出畸形的头部,环状的尾巴以及头部和尾巴的细胞膜缺失。此外,观察到年龄依赖性生殖细胞损失。 TUNEL分析表明,这种生殖细胞损失是由凋亡性生殖细胞死亡增加引起的。这些结果表明,HSV1-TK在睾丸中的表达不仅引起异常的精子发生,而且由于细胞凋亡导致生殖细胞的损失。这些发现可能为阐明转基因动物和被HSV感染的患者中男性不育的分子机制提供新线索。

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