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Developmental cell

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Autophagic elimination of ribosomes during spermiogenesis provides energy for flagellar motility

Published:23 August 2021 DOI: 10.1016/j.devcel.2021.07.015 PMID: 34428398
Yuqing Lei, Xueguang Zhang, Qingjia Xu, Shiyan Liu, Chunxia Li, Hui Jiang, Haocheng Lin, Eryan Kong, Jiaming Liu, Shiqian Qi, Huihui Li, Wenming Xu, Kefeng Lu

Abstract

How autophagy initiation is regulated and what the functional significance of this regulation is are unknown. Here, we characterized the role of yeast Vac8 in autophagy initiation through recruitment of PIK3C3-C1 to the phagophore assembly site (PAS). This recruitment is dependent on the palmitoylation of Vac8 and on its middle ARM domains for binding PIK3C3-C1. Vac8-mediated anchoring of PIK3C3-C1 promotes PtdIns3P generation at the PAS and recruitment of the PtdIns3P binding protein Atg18-Atg2. The mouse homolog of Vac8, ARMC3, is conserved and functions in autophagy in mouse testes. Mice lacking ARMC3 have normal viability but show complete male infertility. Proteomic analysis indicated that the autophagic degradation of cytosolic ribosomes was blocked in ARMC3-deficient spermatids, which caused low energy levels of mitochondria and motionless flagella. These studies uncovered a function of Vac8/ARMC3 in PtdIns3-kinase anchoring at the PAS and its physical significance in mammalian spermatogenesis with a germ tissue-specific autophagic function.

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Materials
Procduct Name CAS Molecular Formula Supplier Price
Rapamycin 53123-88-9 C51H79NO13 1040 suppliers $9.00-$6160.00
Rapamycin 53123-88-9 C51H79NO13 1040 suppliers $9.00-$6160.00
Rapamycin 53123-88-9 C51H79NO13 1040 suppliers $9.00-$6160.00
Rapamycin 53123-88-9 C51H79NO13 1040 suppliers $9.00-$6160.00
Rapamycin 53123-88-9 - Inquiry
Rapamycin 53123-88-9 - Inquiry

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