Journal Article10.1038/s41467-023-40537-x
Auranofin targets UBA1 and enhances UBA1 activity by facilitating ubiquitin trans-thioesterification to E2 ubiquitin-conjugating enzymes
Wenjing Yan,Yongwang Zhong,Xin Hu,Tuan Xu,Yinghua Zhang,Stephen C. Kales,Yanyan Qu,Daniel C. Talley,Bolormaa Baljinnyam,Christopher A. LeClair,Anton Simeonov,Brian M. Polster,Ruili Huang,Yihong Ye,Ganesha Rai,Mark J. Henderson,Ding Tao,Shengyun Fang +17 more
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TL;DR: Auranofin, a drug approved for the treatment of rheumatoid arthritis, is a potent UBA1 activity enhancer that promotes ubiquitination and degradation of misfolded ER proteins during ER-associated degradation in cells at low nanomolar concentrations.
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Abstract: Abstract UBA1 is the primary E1 ubiquitin-activating enzyme responsible for generation of activated ubiquitin required for ubiquitination, a process that regulates stability and function of numerous proteins. Decreased or insufficient ubiquitination can cause or drive aging and many diseases. Therefore, a small-molecule enhancing UBA1 activity could have broad therapeutic potential. Here we report that auranofin, a drug approved for the treatment of rheumatoid arthritis, is a potent UBA1 activity enhancer. Auranofin binds to the UBA1’s ubiquitin fold domain and conjugates to Cys1039 residue. The binding enhances UBA1 interactions with at least 20 different E2 ubiquitin-conjugating enzymes, facilitating ubiquitin charging to E2 and increasing the activities of seven representative E3s in vitro. Auranofin promotes ubiquitination and degradation of misfolded ER proteins during ER-associated degradation in cells at low nanomolar concentrations. It also facilitates outer mitochondrial membrane-associated degradation. These findings suggest that auranofin can serve as a much-needed tool for UBA1 research and therapeutic exploration.
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