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Quality Control Against Misfolded Proteins in the Cytosol: A Network for Cell Survival

Journal

JOURNAL OF BIOCHEMISTRY
Volume 146, Issue 5, Pages 609-616

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/jb/mvp139

Keywords

autophagylysosome system; molecular chaperone; protein misfolding; protein quality control; ubiquitinproteasome system

Funding

  1. Ministry of Education, Culture, Sports, Science and Technology of Japan
  2. Japanese Society for the Promotion of Science

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Misfolded proteins are toxic to cells and the accumulation of toxic species can lead to protein misfolding diseases, such as neurodegenerative disorders. The toxicity of misfolded proteins is thought to result from the presence of exposed hydrophobic surfaces, which mediate unnecessary binding to normal proteins, interrupting essential interactions between cellular proteins. To prevent toxicity, quality control systems monitor protein folding and remove misfolded species in the cytosol. Molecular chaperones recognize and mask hydrophobic surfaces of misfolded monomers, and transfer them to the ubiquitinproteasome system and chaperone-mediated autophagy. To eliminate soluble aggregates of misfolded proteins, the macroautophagylysosome system is thought to degrade proteasome-resistant toxic species. In addition, the microtubule-dependent transport system sequesters soluble oligomers/aggregates into inclusion bodies. These systems are regulated by stress-inducible transcription factors, cochaperones and other cofactors for the effective removal of toxic monomers and oligomers. This review explores the roles of protein quality control pathways and networks that control quality control activities in the cytosol, particularly focusing on recent progress in this field.

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