DNAJB12 and Hsp70 triage arrested intermediates of N1303K-CFTR for endoplasmic reticulum-associated autophagy

The transmembrane Hsp40 DNAJB12 and cytosolic Hsp70 cooperate on the endoplasmic reticulum's (ER) cytoplasmic face to facilitate the triage of nascent polytopic membrane proteins for folding versus degradation. N1303K is a common mutation that causes misfolding of the ion channel CFTR, but unli...

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Veröffentlicht in:	Molecular biology of the cell 2021-04, Vol.32 (7), p.538-553
Hauptverfasser:	He, Lihua, Kennedy, Andrew S, Houck, Scott, Aleksandrov, Andrei, Quinney, Nancy L, Cyr-Scully, Alexandra, Cholon, Deborah M, Gentzsch, Martina, Randell, Scott H, Ren, Hong Yu, Cyr, Douglas M
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Schlagworte:	Animals Autophagosomes Autophagy - physiology Cell Line Chlorocebus aethiops COS Cells Cricetinae Cystic Fibrosis Transmembrane Conductance Regulator - metabolism Cystic Fibrosis Transmembrane Conductance Regulator - physiology Endoplasmic Reticulum - metabolism Endoplasmic Reticulum-Associated Degradation - physiology Heat-Shock Proteins - metabolism HEK293 Cells HSP40 Heat-Shock Proteins - genetics HSP40 Heat-Shock Proteins - metabolism HSP40 Heat-Shock Proteins - physiology HSP70 Heat-Shock Proteins - metabolism Humans Protein Folding
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container_title	Molecular biology of the cell
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creator	He, Lihua Kennedy, Andrew S Houck, Scott Aleksandrov, Andrei Quinney, Nancy L Cyr-Scully, Alexandra Cholon, Deborah M Gentzsch, Martina Randell, Scott H Ren, Hong Yu Cyr, Douglas M
description	The transmembrane Hsp40 DNAJB12 and cytosolic Hsp70 cooperate on the endoplasmic reticulum's (ER) cytoplasmic face to facilitate the triage of nascent polytopic membrane proteins for folding versus degradation. N1303K is a common mutation that causes misfolding of the ion channel CFTR, but unlike F508del-CFTR, biogenic and functional defects in N1303K-CFTR are resistant to correction by folding modulators. N1303K is reported to arrest CFTR folding at a late stage after partial assembly of its N-terminal domains. N1303K-CFTR intermediates are clients of JB12-Hsp70 complexes, maintained in a detergent-soluble state, and have a relatively long 3-h half-life. ER-associated degradation (ERAD)-resistant pools of N1303K-CFTR are concentrated in ER tubules that associate with autophagy initiation sites containing WIPI1, FlP200, and LC3. Destabilization of N1303K-CFTR or depletion of JB12 prevents entry of N1303K-CFTR into the membranes of ER-connected phagophores and traffic to autolysosomes. In contrast, the stabilization of intermediates with the modulator VX-809 promotes the association of N1303K-CFTR with autophagy initiation machinery. N1303K-CFTR is excluded from the ER-exit sites, and its passage from the ER to autolysosomes does not require ER-phagy receptors. DNAJB12 operates in biosynthetically active ER microdomains to triage membrane protein intermediates in a conformation-specific manner for secretion versus degradation via ERAD or selective-ER-associated autophagy.
doi_str_mv	10.1091/mbc.E20-11-0688
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N1303K is a common mutation that causes misfolding of the ion channel CFTR, but unlike F508del-CFTR, biogenic and functional defects in N1303K-CFTR are resistant to correction by folding modulators. N1303K is reported to arrest CFTR folding at a late stage after partial assembly of its N-terminal domains. N1303K-CFTR intermediates are clients of JB12-Hsp70 complexes, maintained in a detergent-soluble state, and have a relatively long 3-h half-life. ER-associated degradation (ERAD)-resistant pools of N1303K-CFTR are concentrated in ER tubules that associate with autophagy initiation sites containing WIPI1, FlP200, and LC3. Destabilization of N1303K-CFTR or depletion of JB12 prevents entry of N1303K-CFTR into the membranes of ER-connected phagophores and traffic to autolysosomes. In contrast, the stabilization of intermediates with the modulator VX-809 promotes the association of N1303K-CFTR with autophagy initiation machinery. 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N1303K is a common mutation that causes misfolding of the ion channel CFTR, but unlike F508del-CFTR, biogenic and functional defects in N1303K-CFTR are resistant to correction by folding modulators. N1303K is reported to arrest CFTR folding at a late stage after partial assembly of its N-terminal domains. N1303K-CFTR intermediates are clients of JB12-Hsp70 complexes, maintained in a detergent-soluble state, and have a relatively long 3-h half-life. ER-associated degradation (ERAD)-resistant pools of N1303K-CFTR are concentrated in ER tubules that associate with autophagy initiation sites containing WIPI1, FlP200, and LC3. Destabilization of N1303K-CFTR or depletion of JB12 prevents entry of N1303K-CFTR into the membranes of ER-connected phagophores and traffic to autolysosomes. In contrast, the stabilization of intermediates with the modulator VX-809 promotes the association of N1303K-CFTR with autophagy initiation machinery. 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subjects	Animals Autophagosomes Autophagy - physiology Cell Line Chlorocebus aethiops COS Cells Cricetinae Cystic Fibrosis Transmembrane Conductance Regulator - metabolism Cystic Fibrosis Transmembrane Conductance Regulator - physiology Endoplasmic Reticulum - metabolism Endoplasmic Reticulum-Associated Degradation - physiology Heat-Shock Proteins - metabolism HEK293 Cells HSP40 Heat-Shock Proteins - genetics HSP40 Heat-Shock Proteins - metabolism HSP40 Heat-Shock Proteins - physiology HSP70 Heat-Shock Proteins - metabolism Humans Protein Folding
title	DNAJB12 and Hsp70 triage arrested intermediates of N1303K-CFTR for endoplasmic reticulum-associated autophagy
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