Literature DB >> 25342745

The molecular chaperone TRiC/CCT binds to the Trp-Asp 40 (WD40) repeat protein WDR68 and promotes its folding, protein kinase DYRK1A binding, and nuclear accumulation.

Yoshihiko Miyata1, Takeshi Shibata2, Masato Aoshima2, Takuichi Tsubata2, Eisuke Nishida3.   

Abstract

Trp-Asp (WD) repeat protein 68 (WDR68) is an evolutionarily conserved WD40 repeat protein that binds to several proteins, including dual specificity tyrosine phosphorylation-regulated protein kinase (DYRK1A), MAPK/ERK kinase kinase 1 (MEKK1), and Cullin4-damage-specific DNA-binding protein 1 (CUL4-DDB1). WDR68 affects multiple and diverse physiological functions, such as controlling anthocyanin synthesis in plants, tissue growth in insects, and craniofacial development in vertebrates. However, the biochemical basis and the regulatory mechanism of WDR68 activity remain largely unknown. To better understand the cellular function of WDR68, here we have isolated and identified cellular WDR68 binding partners using a phosphoproteomic approach. More than 200 cellular proteins with wide varieties of biochemical functions were identified as WDR68-binding protein candidates. Eight T-complex protein 1 (TCP1) subunits comprising the molecular chaperone TCP1 ring complex/chaperonin-containing TCP1 (TRiC/CCT) were identified as major WDR68-binding proteins, and phosphorylation sites in both WDR68 and TRiC/CCT were identified. Co-immunoprecipitation experiments confirmed the binding between TRiC/CCT and WDR68. Computer-aided structural analysis suggested that WDR68 forms a seven-bladed β-propeller ring. Experiments with a series of deletion mutants in combination with the structural modeling showed that three of the seven β-propeller blades of WDR68 are essential and sufficient for TRiC/CCT binding. Knockdown of cellular TRiC/CCT by siRNA caused an abnormal WDR68 structure and led to reduction of its DYRK1A-binding activity. Concomitantly, nuclear accumulation of WDR68 was suppressed by the knockdown of TRiC/CCT, and WDR68 formed cellular aggregates when overexpressed in the TRiC/CCT-deficient cells. Altogether, our results demonstrate that the molecular chaperone TRiC/CCT is essential for correct protein folding, DYRK1A binding, and nuclear accumulation of WDR68.
© 2014 by The American Society for Biochemistry and Molecular Biology, Inc.

Entities:  

Keywords:  DYRK1A; Heat Shock Protein (HSP); Molecular Chaperone; Nuclear Translocation; Phosphoproteomics; Protein Phosphorylation; TCP1; TRiC/CCT; WD40 Repeat; WDR68

Mesh:

Substances:

Year:  2014        PMID: 25342745      PMCID: PMC4246089          DOI: 10.1074/jbc.M114.586115

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  65 in total

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  16 in total

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2.  Biochemical Reduction of the Topology of the Diverse WDR76 Protein Interactome.

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Journal:  J Proteome Res       Date:  2019-08-09       Impact factor: 4.466

Review 3.  The ATP-powered gymnastics of TRiC/CCT: an asymmetric protein folding machine with a symmetric origin story.

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Journal:  Curr Opin Struct Biol       Date:  2019-04-09       Impact factor: 6.809

4.  Nascent Polypeptide Domain Topology and Elongation Rate Direct the Cotranslational Hierarchy of Hsp70 and TRiC/CCT.

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5.  DCAF7 is required for maintaining the cellular levels of ERCC1-XPF and nucleotide excision repair.

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6.  The adaptor protein DCAF7 mediates the interaction of the adenovirus E1A oncoprotein with the protein kinases DYRK1A and HIPK2.

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7.  The TRiC chaperonin controls reovirus replication through outer-capsid folding.

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9.  Chaperonin CCT checkpoint function in basal transcription factor TFIID assembly.

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Journal:  Nat Struct Mol Biol       Date:  2018-12-03       Impact factor: 15.369

10.  Interaction with the CCT chaperonin complex limits APOBEC3A cytidine deaminase cytotoxicity.

Authors:  Abby M Green; Rachel A DeWeerd; David R O'Leary; Ava R Hansen; Katharina E Hayer; Katarzyna Kulej; Ariel S Dineen; Julia H Szeto; Benjamin A Garcia; Matthew D Weitzman
Journal:  EMBO Rep       Date:  2021-08-04       Impact factor: 9.071

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