ESCRTs and associated proteins in lysosomal fusion with endosomes and autophagosomes.

P. Majumder, Oishee Chakrabarti
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引用次数: 3

Abstract

Endolysosomal and autophagosomal degradation pathways are highly connected at various levels, sharing multiple molecular effectors that modulate them individually or simultaneously. These two lysosomal degradative pathways are primarily involved in the disposal of cargo internalized from the cell surface or long-lived proteins or aggregates and aged organelles present in the cytosol. Both of these pathways involve a number of carefully regulated vesicular fusion events that are dependent on ESCRT proteins. The ESCRT proteins especially ESCRT-I and III participate in the regulation of fusion events between autophagosome/amphisome and lysosome. Along with these, a number of functionally diverse ESCRT associated and regulatory proteins such as, endosomal PtdIns (3) P 5-kinase Fab1, ALIX, mahogunin ring finger 1, atrogin 1, syntaxin 17, ATG12-ATG3 complex, and protein kinase CK2α are involved in fusion events in either or both the lysosomal degradative pathways.
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escrt和溶酶体与核内体和自噬体融合的相关蛋白。
内溶酶体和自噬体降解途径在不同水平上高度连接,共享多个单独或同时调节它们的分子效应。这两种溶酶体降解途径主要涉及处理细胞表面内化的货物或存在于细胞质中的长寿命蛋白质或聚集体和老化细胞器。这两种途径都涉及许多依赖于ESCRT蛋白的精心调节的囊泡融合事件。ESCRT蛋白特别是ESCRT- i和ESCRT- III参与调节自噬体/两性体与溶酶体之间的融合事件。除此之外,许多功能多样的ESCRT相关蛋白和调节蛋白,如内体PtdIns (3) p5 -kinase Fab1、ALIX、mahogunin ring finger 1、atrogin 1、syntaxin 17、ATG12-ATG3复合物和蛋白激酶CK2α都参与溶酶体降解途径中的融合事件。
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