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• W4317820218 abstract "Abstract Despite significant progress in clinical management, drug resistance remains a major obstacle. Recent research based on protein degradation to restrain drug resistance has attracted wide attention, and several therapeutic strategies such as inhibition of proteasome with bortezomib and proteolysis-targeting chimeric have been developed. Compared with intervention at the transcriptional level, targeting the degradation process seems to be a more rapid and direct strategy. Proteasomal proteolysis and lysosomal proteolysis are the most critical quality control systems responsible for the degradation of proteins or organelles. Although proteasomal and lysosomal inhibitors (e.g., bortezomib and chloroquine) have achieved certain improvements in some clinical application scenarios, their routine application in practice is still a long way off, which is due to the lack of precise targeting capabilities and inevitable side effects. In-depth studies on the regulatory mechanism of critical protein degradation regulators, including E3 ubiquitin ligases, deubiquitylating enzymes (DUBs), and chaperones, are expected to provide precise clues for developing targeting strategies and reducing side effects. Here, we discuss the underlying mechanisms of protein degradation in regulating drug efflux, drug metabolism, DNA repair, drug target alteration, downstream bypass signaling, sustaining of stemness, and tumor microenvironment remodeling to delineate the functional roles of protein degradation in drug resistance. We also highlight specific E3 ligases, DUBs, and chaperones, discussing possible strategies modulating protein degradation to target cancer drug resistance. A systematic summary of the molecular basis by which protein degradation regulates tumor drug resistance will help facilitate the development of appropriate clinical strategies." @default.
• W4317820218 created "2023-01-24" @default.
• W4317820218 creator A5014538004 @default.
• W4317820218 creator A5021471823 @default.
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• W4317820218 creator A5043883660 @default.
• W4317820218 creator A5056106013 @default.
• W4317820218 creator A5063613049 @default.
• W4317820218 creator A5074509852 @default.
• W4317820218 creator A5078714779 @default.
• W4317820218 date "2023-01-24" @default.
• W4317820218 modified "2023-10-17" @default.
• W4317820218 title "Protein degradation: expanding the toolbox to restrain cancer drug resistance" @default.
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