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An ATG12‐ATG5‐TECPR1 E3‐like complex regulates unconventional LC3 lipidation at damaged lysosomes

Dale Corkery, Sergio Castro‐Gonzalez, Anastasia Knyazeva, Laura K. Herzog, Yao‐Wen Wu

2023EMBO Reports68 citationsDOIOpen Access PDF

Abstract

Lysosomal membrane damage represents a threat to cell viability. As such, cells have evolved sophisticated mechanisms to maintain lysosomal integrity. Small membrane lesions are detected and repaired by the endosomal sorting complex required for transport (ESCRT) machinery while more extensively damaged lysosomes are cleared by a galectin-dependent selective macroautophagic pathway (lysophagy). In this study, we identify a novel role for the autophagosome-lysosome tethering factor, TECPR1, in lysosomal membrane repair. Lysosomal damage promotes TECPR1 recruitment to damaged membranes via its N-terminal dysferlin domain. This recruitment occurs upstream of galectin and precedes the induction of lysophagy. At the damaged membrane, TECPR1 forms an alternative E3-like conjugation complex with the ATG12-ATG5 conjugate to regulate ATG16L1-independent unconventional LC3 lipidation. Abolishment of LC3 lipidation via ATG16L1/TECPR1 double knockout impairs lysosomal recovery following damage.

Topics & Concepts

Lipid-anchored proteinCell biologyATG5AutophagosomeAutophagyEndosomeLysosomeESCRTATG16L1BiologyTFEBTSG101Endocytic cycleChemistryIntracellularCellEndocytosisBiochemistryApoptosisMicrovesiclesEnzymemicroRNAGeneAutophagy in Disease and TherapyCalcium signaling and nucleotide metabolismLysosomal Storage Disorders Research
An ATG12‐ATG5‐TECPR1 E3‐like complex regulates unconventional LC3 lipidation at damaged lysosomes | Litcius