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睾丸特异性bZip型转录因子Tisp40在精子发生过程中的内质网应激反应和染色质包装中发挥作用。

The testes-specific bZip type transcription factor Tisp40 plays a role in ER stress responses and chromatin packaging during spermiogenesis.

作者信息

Nagamori Ippei, Yomogida Kentaro, Ikawa Masahito, Okabe Masaru, Yabuta Norikazu, Nojima Hiroshi

机构信息

Department of Molecular Genetics, Research Institute for Microbial Diseases, Osaka University, Yamadaoka 3-1, Suita City, Osaka 565-0871, Japan.

出版信息

Genes Cells. 2006 Oct;11(10):1161-71. doi: 10.1111/j.1365-2443.2006.01013.x.

Abstract

We previously reported that the spermatid-specific transcription factor Tisp40 functions through UPRE and CRE. To investigate Tisp40 function in vivo, we generated TISP40(-/-) mice. TISP40(-/-) mice were born at expected ratios, were healthy, and mutant males bred normally. However, the ER stress-response protein Grp78/BiP accumulated in the TISP40(-/-) testis and RAMP4 (Ribosome-associated membrane protein 4) mRNA level was up-regulated. Disruption of TISP40 caused ER stress and activation of caspase 12 but not caspase 9, leading to apoptosis of meiotic/postmeiotic germ cells. On the other hand, DAPI staining and electron microscopy revealed that epididymal sperm nuclei were abnormally relaxed in the TISP40(-/-) testis, a phenotype that was independent of the expression and maturation of transition proteins and protamines but due to abnormally retained histones. Histones localized to the cytoplasm as well as to the nucleus and were also retained in epididymal sperm. Histones H2A and H4 were dramatically up-regulated and the acetylation of H2A, H2B and H4 was also enhanced in the TISP40(-/-) testis. Taken together, we conclude that Tisp40 plays an important role in the unfolded protein response of the testis and in regulating the maturation of sperm head nuclei.

摘要

我们之前报道过,精子细胞特异性转录因子Tisp40通过UPRE和CRE发挥作用。为了研究Tisp40在体内的功能,我们培育了TISP40(-/-)小鼠。TISP40(-/-)小鼠以预期比例出生,健康且突变雄性繁殖正常。然而,内质网应激反应蛋白Grp78/BiP在TISP40(-/-)睾丸中积累,且RAMP4(核糖体相关膜蛋白4)mRNA水平上调。TISP40的缺失导致内质网应激和半胱天冬酶12而非半胱天冬酶9的激活,从而导致减数分裂/减数分裂后生殖细胞凋亡。另一方面,DAPI染色和电子显微镜显示,TISP40(-/-)睾丸中附睾精子核异常松弛,这种表型与过渡蛋白和鱼精蛋白的表达及成熟无关,而是由于组蛋白异常保留。组蛋白定位于细胞质以及细胞核中,并且也保留在附睾精子中。在TISP40(-/-)睾丸中,组蛋白H2A和H4显著上调,H2A、H2B和H4的乙酰化也增强。综上所述,我们得出结论,Tisp40在睾丸的未折叠蛋白反应以及调节精子头部细胞核成熟中起重要作用。

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