Journal
AUTOPHAGY
Volume 18, Issue 4, Pages 937-938Publisher
TAYLOR & FRANCIS INC
DOI: 10.1080/15548627.2022.2030175
Keywords
ER structure; Lunapark; misfolded prohormones and neuropeptides; protein quality control; reticulophagy; SEC24C
Categories
Funding
- NIGMS [R35GM131681]
- NINDS [R01NS117440]
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The research reveals that misfolded proteins can be targeted to lysosomes for degradation through the reticulophagy pathway. Furthermore, harmful cargoes with fluid-like behavior are segregated into tubular structures to prevent expansion and impact on cell health.
The endoplasmic reticulum (ER) forms a contiguous network of tubules and sheets. When errors in protein folding occur, misfolded proteins accumulate in the ER. Proteostasis can be restored by ER quality control pathways. Reticulophagy is an ER quality control pathway that uses resident autophagy receptors to link an ER domain to the autophagy machinery. We recently showed that the reticulophagy receptor RTN3L recruits the COPII cargo adaptor SEC24C to target disease-causing mutant proinsulin INS2(Akita) puncta to the lysosome for degradation. When reticulophagy is disrupted and delivery to the lysosome is blocked, large INS2(Akita) puncta accumulate in the ER. Photobleach analysis revealed that these puncta behave like liquid condensates and not aggregates, as previously suggested. Other reticulophagy substrates that are segregated into tubules behave like INS2(Akita), whereas a substrate of the ER sheets receptor, RETREG1/FAM134B, appears to be less fluid. Large INS2(Akita) puncta also accumulate when ER sheets are proliferated by the loss of LNPK, or by overproduction of the sheets-producing protein, CKAP4/CLIMP63. Restoring the tubular network by overexpressing reticulons reverses this phenotype. Our findings revealed that fluid-like deleterious cargoes are segregated into tubules to prevent them from expanding and affecting cell health while they are waiting to undergo reticulophagy.
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