| Literature DB >> 28003215 |
Chao Liu1, Zhenhua Song1,2,3, Lina Wang1,2, Haiyan Yu1,2, Weixiao Liu1, Yongliang Shang1,2, Zhiliang Xu1,2, Haichao Zhao1,2, Fengyi Gao1, Jiamin Wen1,2, Linan Zhao1, Yaoting Gui4, Jianwei Jiao1, Fei Gao1, Wei Li5.
Abstract
Sirt1 is a member of the sirtuin family of proteins and has important roles in numerous biological processes. Sirt1-/- mice display an increased frequency of abnormal spermatozoa, but the mechanism of Sirt1 in spermiogenesis remains largely unknown. Here, we report that Sirt1 might be directly involved in spermiogenesis in germ cells but not in steroidogenic cells. Germ cell-specific Sirt1 knockout mice were almost completely infertile; the early mitotic and meiotic progression of germ cells in spermatogenesis were not obviously affected after Sirt1 depletion, but subsequent spermiogenesis was disrupted by a defect in acrosome biogenesis, which resulted in a phenotype similar to that observed in human globozoospermia. In addition, LC3 and Atg7 deacetylation was disrupted in spermatids after knocking out Sirt1, which affected the redistribution of LC3 from the nucleus to the cytoplasm and the activation of autophagy. Furthermore, Sirt1 depletion resulted in the failure of LC3 to be recruited to Golgi apparatus-derived vesicles and in the failure of GOPC and PICK1 to be recruited to nucleus-associated acrosomal vesicles. Taken together, these findings reveal that Sirt1 has a novel physiological function in acrosome biogenesis.Entities:
Keywords: Acrosome biogenesis; Autophagy; Deacetylation; Globozoospermia; Map1lc3; Mouse; Sirt1
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Year: 2016 PMID: 28003215 DOI: 10.1242/dev.147074
Source DB: PubMed Journal: Development ISSN: 0950-1991 Impact factor: 6.868