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未闭合的自噬体进入液泡及其生理相关性。

The entry of unclosed autophagosomes into vacuoles and its physiological relevance.

机构信息

College of Life Sciences, Key Laboratory of Agricultural Environmental Microbiology of Ministry of Agriculture and Rural Affairs, Nanjing Agricultural University, Nanjing, China.

National Laboratory of Biomacromolecules, CAS Center for Excellence in Biomacromolecules, Institute of Biophysics, Chinese Academy of Sciences, Beijing, China.

出版信息

PLoS Genet. 2022 Oct 13;18(10):e1010431. doi: 10.1371/journal.pgen.1010431. eCollection 2022 Oct.

Abstract

It is widely stated in the literature that closed mature autophagosomes (APs) fuse with lysosomes/vacuoles during macroautophagy/autophagy. Previously, we showed that unclosed APs accumulated as clusters outside vacuoles in Vps21/Rab5 and ESCRT mutants after a short period of nitrogen starvation. However, the fate of such unclosed APs remains unclear. In this study, we used a combination of cellular and biochemical approaches to show that unclosed double-membrane APs entered vacuoles and formed unclosed single-membrane autophagic bodies after prolonged nitrogen starvation or rapamycin treatment. Vacuolar hydrolases, vacuolar transport chaperon (VTC) proteins, Ypt7, and Vam3 were all involved in the entry of unclosed double-membrane APs into vacuoles in Vps21-mutant cells. Overexpression of the vacuolar hydrolases, Pep4 or Prb1, or depletion of most VTC proteins promoted the entry of unclosed APs into vacuoles in Vps21-mutant cells, whereas depletion of Pep4 and/or Prb1 delayed the entry into vacuoles. In contrast to the complete infertility of diploid cells of typical autophagy mutants, diploid cells of Vps21 mutant progressed through meiosis to sporulation, benefiting from the entry of unclosed APs into vacuoles after prolonged nitrogen starvation. Overall, these data represent a new observation that unclosed double-membrane APs can enter vacuoles after prolonged autophagy induction, most likely as a survival strategy.

摘要

文献中广泛指出,在巨自噬/自噬过程中,闭合成熟的自噬体(AP)与溶酶体/液泡融合。此前,我们发现,在氮饥饿后很短的时间内,未闭合的 AP 在 Vps21/Rab5 和 ESCRT 突变体中外膜与液泡融合,并聚集在外膜与液泡之间。然而,这种未闭合的 AP 的命运尚不清楚。在这项研究中,我们使用细胞和生化方法的组合表明,在长时间氮饥饿或雷帕霉素处理后,未闭合的双层膜 AP 进入液泡,并形成未闭合的单层自噬体。液泡水解酶、液泡运输伴侣(VTC)蛋白、Ypt7 和 Vam3 均参与了未闭合双层膜 AP 进入 Vps21 突变细胞液泡的过程。液泡水解酶 Pep4 或 Prb1 的过表达或大多数 VTC 蛋白的消耗促进了未闭合 AP 进入 Vps21 突变细胞液泡,而 Pep4 和/或 Prb1 的消耗则延迟了进入液泡的时间。与典型自噬突变体二倍体细胞完全不育相反,Vps21 突变体的二倍体细胞经过减数分裂到孢子形成,得益于长时间氮饥饿后未闭合 AP 进入液泡。总的来说,这些数据代表了一个新的观察结果,即未闭合的双层膜 AP 在长时间自噬诱导后可以进入液泡,这很可能是一种生存策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1465/9562215/1ca8099ee250/pgen.1010431.g001.jpg

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