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Nphp1基因的靶向破坏会导致小鼠精子形态发生后期步骤出现缺陷,从而引起雄性不育。

Targeted disruption of Nphp1 causes male infertility due to defects in the later steps of sperm morphogenesis in mice.

作者信息

Jiang Si-Tse, Chiou Yuan-Yow, Wang Ellian, Lin Hsiu-Kuan, Lee Sue-Ping, Lu Hsin-Yi, Wang Chi-Kuang Leo, Tang Ming-Jer, Li Hung

机构信息

Institute of Molecular Biology, Academia Sinica, Taipei 115, Taiwan.

出版信息

Hum Mol Genet. 2008 Nov 1;17(21):3368-79. doi: 10.1093/hmg/ddn231. Epub 2008 Aug 5.

Abstract

Juvenile nephronophthisis type I is the most common genetic disorder causing end-stage renal failure in children and young adults. The defective gene responsible has been identified as NPHP1. Its gene product, nephrocystin-1, is a novel protein of uncertain function that is widely expressed in many tissues and not just confined to the kidney. To gain insight into the physiological function of nephrocystin, Nphp1-targeted mutant mice were generated by homologous recombination. Interestingly, homozygous Nphp1 mutant mice were viable without renal manifestations of nephronophthisis. They appeared normal, but males were infertile with oligoteratozoospermia. Histological analysis of the seminiferous tubules showed that spermatogenesis was blocked at the early stages of spermatid elongation, with degenerating spermatids sloughing off into the lumen. Electron microscopic analysis revealed detachment of early elongating spermatids from Sertoli cells, and a failure of sperm head and tail morphogenesis. However, a few mature spermatozoa were still deposited in the epididymis, though they were frequently dead, immotile, or malformed. These novel findings indicate that nephrocystin is critically required for the differentiation of early elongating spermatids into spermatozoa in mice. The possible roles of nephrocystin in the formation and maintenance of Sertoli-spermatid junctions are still under investigation.

摘要

I型青少年肾单位肾痨是导致儿童和青年终末期肾衰竭的最常见遗传性疾病。已确定致病缺陷基因是NPHP1。其基因产物肾囊肿蛋白-1是一种功能不明的新型蛋白质,广泛表达于许多组织,而不仅限于肾脏。为深入了解肾囊肿蛋白的生理功能,通过同源重组构建了Nphp1靶向突变小鼠。有趣的是,纯合Nphp1突变小鼠存活,无肾单位肾痨的肾脏表现。它们看起来正常,但雄性不育,精子数量少且畸形。对生精小管的组织学分析表明,精子发生在精子细胞伸长的早期阶段受阻,退化的精子细胞脱落到管腔中。电子显微镜分析显示早期伸长的精子细胞与支持细胞分离,精子头部和尾部形态发生失败。然而,仍有一些成熟精子沉积在附睾中,尽管它们经常是死亡的、无运动能力的或畸形的。这些新发现表明,肾囊肿蛋白对小鼠早期伸长的精子细胞分化为精子至关重要。肾囊肿蛋白在支持细胞-精子细胞连接的形成和维持中的可能作用仍在研究中。

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