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P63017

Heat shock cognate 71 kDa protein (P63017)

Uniprot ID P63017
Protein Name Heat shock cognate 71 kDa protein
Gene Name Hspa8
Species Mus musculus (Mouse)
Basic Information Experiments (5) Disease (0) Interactions
Signal peptide(a) N Secretome P(b) 0.347
Function Molecular chaperone implicated in a wide variety of cellular processes, including protection of the proteome from stress, folding and transport of newly synthesized polypeptides, activation of proteolysis of misfolded proteins and the formation and dissociation of protein complexes. Plays a pivotal role in the protein quality control system, ensuring the correct folding of proteins, the re-folding of misfolded proteins and controlling the targeting of proteins for subsequent degradation. This is achieved through cycles of ATP binding, ATP hydrolysis and ADP release, mediated by co-chaperones. The co-chaperones have been shown to not only regulate different steps of the ATPase cycle of HSP70, but they also have an individual specificity such that one co-chaperone may promote folding of a substrate while another may promote degradation. The affinity of HSP70 for polypeptides is regulated by its nucleotide bound state. In the ATP-bound form, it has a low affinity for substrate proteins. However, upon hydrolysis of the ATP to ADP, it undergoes a conformational change that increases its affinity for substrate proteins. HSP70 goes through repeated cycles of ATP hydrolysis and nucleotide exchange, which permits cycles of substrate binding and release. The HSP70-associated co-chaperones are of three types: J-domain co-chaperones HSP40s (stimulate ATPase hydrolysis by HSP70), the nucleotide exchange factors (NEF) such as BAG1/2/3 (facilitate conversion of HSP70 from the ADP-bound to the ATP-bound state thereby promoting substrate release), and the TPR domain chaperones such as HOPX and STUB1. Acts as a repressor of transcriptional activation. Inhibits the transcriptional coactivator activity of CITED1 on Smad-mediated transcription. Component of the PRP19-CDC5L complex that forms an integral part of the spliceosome and is required for activating pre-mRNA splicing. May have a scaffolding role in the spliceosome assembly as it contacts all other components of the core complex. Binds bacterial lipopolysaccharide (LPS) and mediates LPS-induced inflammatory response, including TNF secretion. Participates in the ER-associated degradation (ERAD) quality control pathway in conjunction with J domain-containing co-chaperones and the E3 ligase STUB1. .
GO - Molecular function
  • A1 adenosine receptor binding : ISO:MGI
  • ADP binding : ISO:MGI
  • ATP binding : ISO:MGI
  • ATPase activity : ISO:MGI
  • ATPase activity, coupled : IDA:MGI
  • C3HC4-type RING finger domain binding : ISO:MGI
  • cadherin binding : ISO:MGI
  • chaperone binding : ISO:MGI
  • clathrin-uncoating ATPase activity : ISO:MGI
  • enzyme binding : ISO:MGI
  • G-protein coupled receptor binding : ISO:MGI
  • heat shock protein binding : ISO:MGI
  • peptide binding : ISO:MGI
  • phosphatidylserine binding : IDA:ParkinsonsUK-UCL
  • prostaglandin binding : ISO:MGI
  • protein binding, bridging : ISO:MGI
  • RNA binding : ISO:MGI
  • signaling receptor binding : ISO:MGI
  • transcription factor binding : ISO:MGI
  • ubiquitin protein ligase binding : ISO:MGI
  • unfolded protein binding : IPI:MGI
GO - Biological process
  • ATP metabolic process : ISO:MGI
  • cellular protein complex disassembly : ISO:MGI
  • chaperone cofactor-dependent protein refolding : IGI:MGI
  • chaperone-mediated autophagy : ISS:ParkinsonsUK-UCL
  • chaperone-mediated autophagy translocation complex disassembly : ISS:ParkinsonsUK-UCL
  • chaperone-mediated protein folding : ISO:MGI
  • chaperone-mediated protein transport involved in chaperone-mediated autophagy : ISO:MGI
  • clathrin coat disassembly : IGI:MGI
  • late endosomal microautophagy : IMP:ParkinsonsUK-UCL
  • modulation by host of viral process : IMP:AgBase
  • mRNA processing : IEA:UniProtKB-KW
  • negative regulation of cardiac muscle cell apoptotic process : ISO:MGI
  • negative regulation of supramolecular fiber organization : ISO:MGI
  • negative regulation of transcription, DNA-templated : ISS:UniProtKB
  • positive regulation by host of viral genome replication : IMP:AgBase
  • positive regulation of catalytic activity : ISO:MGI
  • positive regulation of gene expression : ISO:MGI
  • positive regulation of lysosomal membrane permeability : ISO:MGI
  • positive regulation of mRNA splicing, via spliceosome : IMP:MGI
  • positive regulation of phagocytosis : ISO:MGI
  • positive regulation of protein refolding : ISO:MGI
  • positive regulation of proteolysis : ISO:MGI
  • positive regulation of T cell mediated cytotoxicity : ISO:MGI
  • protein autophosphorylation : ISO:MGI
  • protein folding : IDA:MGI
  • protein import into nucleus : ISO:MGI
  • protein refolding : ISS:ParkinsonsUK-UCL
  • protein targeting to lysosome involved in chaperone-mediated autophagy : ISO:MGI
  • regulation of cell cycle : IDA:MGI
  • regulation of protein complex stability : ISS:ParkinsonsUK-UCL
  • regulation of protein stability : ISO:MGI
  • RNA splicing : IEA:UniProtKB-KW
  • transcription, DNA-templated : IEA:UniProtKB-KW
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(a) The Signal peptide D-score cutoff for "YES"(having signal peptide) is 0.45.
(b) Non-classically secreted proteins should obtain an NN-score(Neural Networks score) exceeding the normal threshold of 0.5, but not at the same time be predicted to contain a signal peptide.