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An intrinsically disordered protein region encoded by the human disease gene regulates mitophagy

Autophagy. 2022-05; 
Morgan A Gingerich, Xueying Liu, Biaoxin Chai, Gemma L Pearson, Michael P Vincent, Tracy Stromer, Jie Zhu, Vaibhav Sidarala, Aaron Renberg, Debashish Sahu, Daniel J Klionsky, Santiago Schnell, Scott A Soleimanpour
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Proteins, Expression, Isolation and Analysis … isoform (Genscript, OHu02258D) was liberated by BamHI restriction digest, gel purified, and ligated in place of the C terminus of the full-length CLEC16A isoform construct (Genscript, … Get A Quote

摘要

CLEC16A regulates mitochondrial health through mitophagy and is associated with over 20 human diseases. However, the key structural and functional regions of CLEC16A, and their relevance for human disease, remain unknown. Here, we report that a disease-associated CLEC16A variant lacks a C-terminal intrinsically disordered protein region (IDPR) that is critical for mitochondrial quality control. IDPRs comprise nearly half of the human proteome, yet their mechanistic roles in human disease are poorly understood. Using carbon detect NMR, we find that the CLEC16A C terminus lacks secondary structure, validating the presence of an IDPR. Loss of the CLEC16A C-terminal IDPR impairs mitophagy, mitochondrial function, ... More

關鍵詞

Diabetes, NMR, insulin, mitophagy, splicing
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