| Literature DB >> 29652515 |
Jared A M Bard1,2, Ellen A Goodall1,2, Eric R Greene1,2, Erik Jonsson1,2,3, Ken C Dong1,2,3, Andreas Martin1,2,3.
Abstract
As the endpoint for the ubiquitin-proteasome system, the 26S proteasome is the principal proteolytic machine responsible for regulated protein degradation in eukaryotic cells. The proteasome's cellular functions range from general protein homeostasis and stress response to the control of vital processes such as cell division and signal transduction. To reliably process all the proteins presented to it in the complex cellular environment, the proteasome must combine high promiscuity with exceptional substrate selectivity. Recent structural and biochemical studies have shed new light on the many steps involved in proteasomal substrate processing, including recognition, deubiquitination, and ATP-driven translocation and unfolding. In addition, these studies revealed a complex conformational landscape that ensures proper substrate selection before the proteasome commits to processive degradation. These advances in our understanding of the proteasome's intricate machinery set the stage for future studies on how the proteasome functions as a major regulator of the eukaryotic proteome.Entities:
Keywords: 26S proteasome; AAA+ ATPase; deubiquitination; energy-dependent protein degradation; ubiquitin code; ubiquitin receptor
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Year: 2018 PMID: 29652515 PMCID: PMC6422034 DOI: 10.1146/annurev-biochem-062917-011931
Source DB: PubMed Journal: Annu Rev Biochem ISSN: 0066-4154 Impact factor: 23.643