The Role of the Proteasome in Limiting Cellular Stress Associated with Protein Accumulation

Author:

Kragness Kate A.1,Trader Darci J.1ORCID

Affiliation:

1. Department of Pharmaceutical Sciences University of California Irvine California 92617 USA

Abstract

AbstractThe proteasome is comprised of multiple subunits that catalyze the degradation of proteins to maintain cellular homeostasis. The proteasome targets protein substrates by two different pathways. The ubiquitin‐dependent pathway requires proteins to be labeled with a ubiquitin tag to signal for degradation by the 26S isoform of the proteasome. Protein degradation through this pathway declines during age progression. The ubiquitin‐independent pathway utilizes the 20S proteasome isoform. It can degrade misfolded and intrinsically disordered proteins to decrease cellular stress. Age‐related protein accumulation and aggregation can occur due to the decreased activity and expression of the proteasome. Protein accumulation causes increased cellular stress which can contribute to disease progression. Increasing proteasome activity could serve as a solution to eliminating and preventing protein accumulation. Studies have shown the value of the proteasome as a therapeutic entity to mitigate cellular stress. This perspective explores the link between proteasome activity and cellular stress caused by age‐related misfolded protein accumulation.

Funder

Division of Intramural Research, National Institute of Allergy and Infectious Diseases

Publisher

Wiley

Subject

General Chemistry

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