Reference: Rabinovich E, et al. (2002) AAA-ATPase p97/Cdc48p, a cytosolic chaperone required for endoplasmic reticulum-associated protein degradation. Mol Cell Biol 22(2):626-34

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Abstract


Endoplasmic reticulum-associated degradation (ERAD) disposes of aberrant proteins in the secretory pathway. Protein substrates of ERAD are dislocated via the Sec61p translocon from the endoplasmic reticulum to the cytosol, where they are ubiquitinated and degraded by the proteasome. Since the Sec61p channel is also responsible for import of nascent proteins, this bidirectional passage should be coordinated, probably by molecular chaperones. Here we implicate the cytosolic chaperone AAA-ATPase p97/Cdc48p in ERAD. We show the association of mammalian p97 and its yeast homologue Cdc48p in complexes with two respective ERAD substrates, secretory immunoglobulin M in B lymphocytes and 6myc-Hmg2p in yeast. The membrane 6myc-Hmg2p as well as soluble lumenal CPY*, two short-lived ERAD substrates, are markedly stabilized in conditional cdc48 yeast mutants. The involvement of Cdc48p in dislocation is underscored by the accumulation of ERAD substrates in the endoplasmic reticulum when Cdc48p fails to function, as monitored by activation of the unfolded protein response. We propose that the role of p97/Cdc48p in ERAD, provided by its potential unfoldase activity and multiubiquitin binding capacity, is to act at the cytosolic face of the endoplasmic reticulum and to chaperone dislocation of ERAD substrates and present them to the proteasome.

Reference Type
Journal Article | Research Support, Non-U.S. Gov't | Research Support, U.S. Gov't, Non-P.H.S.
Authors
Rabinovich E, Kerem A, Fröhlich KU, Diamant N, Bar-Nun S
Primary Lit For
CDC48 | HRD1
Additional Lit For
HMG2 | CDC48-NPL4-UFD1 AAA ATPase complex | CDC48-NPL4-VMS1 AAA ATPase complex | cdc48-10

Gene Ontology Annotations 1 entry for 1 gene


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Gene/ComplexQualifierGene Ontology TermAnnotation ExtensionEvidenceSourceAssigned On
CDC48involved inERAD pathwayIMPSGD2023-12-16
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Phenotype Annotations 2 entries for 2 genes


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GenePhenotypeExperiment TypeMutant InformationStrain BackgroundChemicalDetails
HRD1protein/peptide accumulation: increased
Reporter: 6Myc-Hmg2p
classical geneticsnull
Allele: hrd1-Δ
OtherTreatment: cycloheximide chase
Details: increased half-life at all temperatures tested
CDC48protein/peptide accumulation: increased
Reporter: 6Myc-Hmg2p
classical geneticsconditional
Allele: cdc48-10
OtherTemperature: elevated temperature, 37 °C
Treatment: cycloheximide chase
Details: increased half-life of Hmg2p (and also CPY*); similar results with cdc48-1 (cs allele) and cdc48-7 (ts allele)
Showing 1 to 2 of 2 entries

Interaction Annotations


Genetic Interactions

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Interactor Interactor Allele Assay Annotation Action Phenotype SGA score P-value Source Reference

Physical Interactions 1 entry for 2 genes

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InteractorInteractorAssayAnnotationActionModification
CDC48HMG2Affinity Capture-Westernmanually curatedHit-BaitNo Modification
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