Allosteric regulation of the 20S proteasome by the Catalytic Core Regulators (CCRs) family

被引:20
|
作者
Deshmukh, Fanindra Kumar [1 ]
Ben-Nissan, Gili [1 ]
Olshina, Maya A. [1 ]
Fuzesi-Levi, Maria G. [1 ]
Polkinghorn, Caley [1 ]
Arkind, Galina [1 ]
Leushkin, Yegor [1 ]
Fainer, Irit [1 ]
Fleishman, Sarel J. [1 ]
Tawfik, Dan [1 ]
Sharon, Michal [1 ]
机构
[1] Weizmann Inst Sci, Dept Biomol Sci, IL-7610001R Rehovot, Israel
基金
以色列科学基金会;
关键词
26S PROTEASOME; MASS-SPECTROMETRY; CRYSTAL-STRUCTURE; BETA-7; SUBUNIT; DEGRADATION; PROTEINS; COMPLEXES; DYNAMICS; BINDING; SYSTEM;
D O I
10.1038/s41467-023-38404-w
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
Controlled degradation of proteins is necessary for ensuring their abundance and sustaining a healthy and accurately functioning proteome. One of the degradation routes involves the uncapped 20S proteasome, which cleaves proteins with a partially unfolded region, including those that are damaged or contain intrinsically disordered regions. This degradation route is tightly controlled by a recently discovered family of proteins named Catalytic Core Regulators (CCRs). Here, we show that CCRs function through an allosteric mechanism, coupling the physical binding of the PSMB4 beta-subunit with attenuation of the complex's three proteolytic activities. In addition, by dissecting the structural properties that are required for CCR-like function, we could recapitulate this activity using a designed protein that is half the size of natural CCRs. These data uncover an allosteric path that does not involve the proteasome's enzymatic subunits but rather propagates through the non-catalytic subunit PSMB4. This way of 20S proteasome-specific attenuation opens avenues for decoupling the 20S and 26S proteasome degradation pathways as well as for developing selective 20S proteasome inhibitors. A family of regulators named Catalytic Core Regulators (CCRs) oversees the function of the 20S proteasome. Here, the authors show that CCRs function through an allosteric mechanism, coupling the physical binding of the PSMB4 beta-subunit with attenuation of the proteasome three proteolytic activities.
引用
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页数:24
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