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An N-terminal-truncated isoform of FAM134B (FAM134B-2) regulates starvation-induced hepatic selective ER-phagy.

Life Sci Alliance. 2019-06; 
KohnoShohei,ShiozakiYuji,KeenanAudrey L,Miyazaki-AnzaiShinobu,MiyazakiMa
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Catalog Antibody 2 mg of lysate and 40 μl of anti-DYKDDDDK G1 Affinity Resin (GenScript) were incubated overnight at 4°C. Resins were washed three times with co-immunoprecipitation buffer. Get A Quote

摘要

Autophagy is a conserved system that adapts to nutrient starvation, after which proteins and organelles are degraded to recycle amino acids in response to starvation. Recently, the ER was added to the list of targets of autophagic degradation. Autophagic degradation pathways of bulk ER and the specific proteins sorted through the ER are considered key mechanisms in maintaining ER homeostasis. Four ER-resident proteins (FAM134B, CCPG1, SEC62, and RTN3) have been identified as ER-resident cargo receptors, which contain LC3-interacting regions. In this study, we identified an N-terminal-truncated isoform of FAM134B (FAM134B-2) that contributes to starvation-induced ER-related autophagy. Hepatic FAM13... More

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