JPDI, a Novel Endoplasmic Reticulum-resident Protein Containing Both a BiP-interacting J-domain and Thioredoxin-like Motifs

Hosoda, Akira; Kimata, Yukio; Tsuru, Akio; Kohno, Kenji

doi:10.1074/jbc.m208346200

Cited by 96 publications

(66 citation statements)

References 41 publications

(52 reference statements)

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“…Surprisingly, mutation of the HPD motif significantly enhanced association of ERdj5 with misfolded SP-C (Supplemental Figure S2A). Further analyses revealed that, in contrast to results of a previous study (Hosoda et al, 2003), the HPD mutation did not alter association of ERdj5 (or ERdj4) with BiP (Supplemental Figure S2C). Therefore, stable complexes of misfolded SP-C, BiP, and ERdj5 formed in the absence of the catalytic activity of ERdj5.…”

Section: Discussioncontrasting

confidence: 53%

“…ERdj5 (DNAJC10/JPDI) is an ER-resident lumenal protein with a canonical C-terminal KDEL retrieval motif, a J domain, and four thioredoxin-like domains (Cunnea et al, 2003;Hosoda et al, 2003). Deletion of the J domain prevented interaction of ERdj5 with both BiP and misfolded SP-C, suggesting that association of ERdj5 with substrate was mediated by BiP.…”

Section: Discussionmentioning

confidence: 99%

“…vitro (Cunnea et al, 2003;Hosoda et al, 2003) may reflect the substrate specificity of ERdj5 or the requirement of a partner protein(s), such as BiP, for unfoldase activity. Alternatively, ERdj5 may act as a redox sensor to identify proteins with unpaired/mispaired cysteines and target them for elimination via ERAD.…”

Section: Discussionmentioning

confidence: 99%

“…ERdj4 and ERdj5 were inserted into pIRES2-EGFP vector (Clontech), BiP was inserted into pcDNA3.1 (Invitrogen, Carlsbad, CA), and ERdj3 was inserted into pCMV6-XL5 (OriGene Technologies, Rockville, MD). The hemagglutinin (HA) tag was added at a position before the C-terminal KDEL in ERdj5 as described previously (Hosoda et al, 2003). Mouse insulin 2-Flag was cloned from mouse pancreatic ␤-cell cDNA using PCR with reverse transcription and inserted into the pIRES2-EGFP vector.…”

Section: Microarray Analyses and Reverse Transcription-polymerase Chamentioning

confidence: 99%

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ERdj4 and ERdj5 Are Required for Endoplasmic Reticulum-associated Protein Degradation of Misfolded Surfactant Protein C

Dong

Bridges

Apsley

et al. 2008

MBoC

144

171

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Mutations in the SFTPC gene associated with interstitial lung disease in human patients result in misfolding, endoplasmic reticulum (ER) retention, and degradation of the encoded surfactant protein C (SP-C) proprotein. In this study, genes specifically induced in response to transient expression of two disease-associated mutations were identified by microarray analyses. Immunoglobulin heavy chain binding protein (BiP) and two heat shock protein 40 family members, endoplasmic reticulum-localized DnaJ homologues ERdj4 and ERdj5, were significantly elevated and exhibited prolonged and specific association with the misfolded proprotein; in contrast, ERdj3 interacted with BiP, but it did not associate with either wild-type or mutant SP-C. Misfolded SP-C, ERdj4, and ERdj5 coprecipitated with p97/VCP indicating that the cochaperones remain associated with the misfolded proprotein until it is dislocated to the cytosol. Knockdown of ERdj4 and ERdj5 expression increased ER retention and inhibited degradation of misfolded SP-C, but it had little effect on the wild-type protein. Transient expression of ERdj4 and ERdj5 in X-box binding protein 1 ؊/؊ mouse embryonic fibroblasts substantially restored rapid degradation of mutant SP-C proprotein, whereas transfection of HPD mutants failed to rescue SP-C endoplasmic reticulum-associated protein degradation. ERdj4 and ERdj5 promote turnover of misfolded SP-C and this activity is dependent on their ability to stimulate BiP ATPase activity.

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Section: Discussioncontrasting

confidence: 53%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Microarray Analyses and Reverse Transcription-polymerase Chamentioning

confidence: 99%

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ERdj4 and ERdj5 Are Required for Endoplasmic Reticulum-associated Protein Degradation of Misfolded Surfactant Protein C

Dong

Bridges

Apsley

et al. 2008

MBoC

144

171

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“…These results point to a new functional assignment for p58 IPK in serving as a BiP cochaperone to optimize protein folding homeostasis in the ER. Because p58 IPK represents one among several (at least five others) ER localized Jdomain proteins that interface with BiP (Feldheim et al, 1992;Brightman et al, 1995;Shen et al, 2002;Hosoda et al, 2003;Shen and Hendershot, 2005), its absence would result in an ER lumen that is only modestly compromised in overall folding capacity. The functional consequences of this slightly lower protein maturation capacity would be obscured under all but the most taxing conditions and can explain each of the following phenotypic observations in cells and animals lacking p58 IPK .…”

Section: Discussionmentioning

confidence: 99%

The Role of p58^IPK in Protecting the Stressed Endoplasmic Reticulum

Rutkowski

Kang

Goodman

et al. 2007

MBoC

190

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The preemptive quality control (pQC) pathway protects cells from acute endoplasmic reticulum (ER) stress by attenuating translocation of nascent proteins despite their targeting to translocons at the ER membrane. Here, we investigate the hypothesis that the DnaJ protein p58 IPK plays an essential role in this process via HSP70 recruitment to the cytosolic face of translocons for extraction of translocationally attenuated nascent chains. Our analyses revealed that the heightened stress sensitivity of p58؊/؊ cells was not due to an impairment of the pQC pathway or elevated ER substrate burden during acute stress. Instead, the lesion was in the protein processing capacity of the ER lumen, where p58 IPK was found to normally reside in association with BiP. ER lumenal p58 IPK could be coimmunoprecipitated with a newly synthesized secretory protein in vitro and stimulated protein maturation upon overexpression in cells. These results identify a previously unanticipated location for p58 IPK in the ER lumen where its putative function as a cochaperone explains the stress-sensitivity phenotype of knockout cells and mice.

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Protein Folding in the Endoplasmic Reticulum

Shen

Chung

Hendershot

2008

Protein Science Encyclopedia

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Originally published in: Protein Folding Handbook. Part II. Edited by Johannes Buchner and Thomas Kiefhaber. Copyright © 2005 Wiley‐VCH Verlag GmbH & Co. KGaA Weinheim. Print ISBN: 3‐527‐30784‐2 The sections in this article are Introduction Bi P Interactions with Unfolded Proteins ER ‐localized Dna J Homologues ER ‐localized Nucleotide‐exchange/releasing Factors Organization and Relative Levels of Chaperones in the ER Regulation of ER Chaperone Levels Disposal of BiP‐associated Proteins That Fail to Fold or Assemble Other Roles of Bi P in the ER Conclusions Acknowledgements

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JPDI, a Novel Endoplasmic Reticulum-resident Protein Containing Both a BiP-interacting J-domain and Thioredoxin-like Motifs

Cited by 96 publications

References 41 publications

ERdj4 and ERdj5 Are Required for Endoplasmic Reticulum-associated Protein Degradation of Misfolded Surfactant Protein C

ERdj4 and ERdj5 Are Required for Endoplasmic Reticulum-associated Protein Degradation of Misfolded Surfactant Protein C

The Role of p58^IPK in Protecting the Stressed Endoplasmic Reticulum

Protein Folding in the Endoplasmic Reticulum

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JPDI, a Novel Endoplasmic Reticulum-resident Protein Containing Both a BiP-interacting J-domain and Thioredoxin-like Motifs

Cited by 96 publications

References 41 publications

ERdj4 and ERdj5 Are Required for Endoplasmic Reticulum-associated Protein Degradation of Misfolded Surfactant Protein C

ERdj4 and ERdj5 Are Required for Endoplasmic Reticulum-associated Protein Degradation of Misfolded Surfactant Protein C

The Role of p58IPK in Protecting the Stressed Endoplasmic Reticulum

Protein Folding in the Endoplasmic Reticulum

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The Role of p58^IPK in Protecting the Stressed Endoplasmic Reticulum