Literature DB >> 25223703

Profiling human protein degradome delineates cellular responses to proteasomal inhibition and reveals a feedback mechanism in regulating proteasome homeostasis.

Tao Yu1, Yonghui Tao1, Meiqiang Yang2, Peng Chen1, Xiaobo Gao1, Yanbo Zhang3, Tao Zhang4, Zi Chen5, Jian Hou6, Yan Zhang7, Kangcheng Ruan2, Hongyan Wang8, Ronggui Hu9.   

Abstract

Global change in protein turnover (protein degradome) constitutes a central part of cellular responses to intrinsic or extrinsic stimuli. However, profiling protein degradome remains technically challenging. Recently, inhibition of the proteasome, e.g., by using bortezomib (BTZ), has emerged as a major chemotherapeutic strategy for treating multiple myeloma and other human malignancies, but systematic understanding of the mechanisms for BTZ drug action and tumor drug resistance is yet to be achieved. Here we developed and applied a dual-fluorescence-based Protein Turnover Assay (ProTA) to quantitatively profile global changes in human protein degradome upon BTZ-induced proteasomal inhibition. ProTA and subsequent network analyses delineate potential molecular basis for BTZ action and tumor drug resistance in BTZ chemotherapy. Finally, combined use of BTZ with drugs targeting the ProTA-identified key genes or pathways in BTZ action reduced BTZ resistance in multiple myeloma cells. Remarkably, BTZ stabilizes proteasome subunit PSMC1 and proteasome assembly factor PSMD10, suggesting a previously under-appreciated mechanism for regulating proteasome homeostasis. Therefore, ProTA is a novel tool for profiling human protein degradome to elucidate potential mechanisms of drug action and resistance, which might facilitate therapeutic development targeting proteostasis to treat human disorders.

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Year:  2014        PMID: 25223703      PMCID: PMC4185348          DOI: 10.1038/cr.2014.122

Source DB:  PubMed          Journal:  Cell Res        ISSN: 1001-0602            Impact factor:   25.617


  72 in total

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2.  Ubiquitylation of p62/sequestosome1 activates its autophagy receptor function and controls selective autophagy upon ubiquitin stress.

Authors:  Hong Peng; Jiao Yang; Guangyi Li; Qing You; Wen Han; Tianrang Li; Daming Gao; Xiaoduo Xie; Byung-Hoon Lee; Juan Du; Jian Hou; Tao Zhang; Hai Rao; Ying Huang; Qinrun Li; Rong Zeng; Lijian Hui; Hongyan Wang; Qin Xia; Xuemin Zhang; Yongning He; Masaaki Komatsu; Ivan Dikic; Daniel Finley; Ronggui Hu
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4.  Quantitative expression of Ikaros, IRF4, and PSMD10 proteins predicts survival in VRD-treated patients with multiple myeloma.

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5.  N-Terminal-Based Targeted, Inducible Protein Degradation in Escherichia coli.

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6.  A genome-scale CRISPR-Cas9 screening method for protein stability reveals novel regulators of Cdc25A.

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