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Molecular basis for the bifunctional Uba4–Urm1 sulfur‐relay system in tRNA thiolation and ubiquitin‐like conjugation

EMBO J. 2020-10; 
Marta Pabis , Martin Termathe , Keerthiraju E Ravichandran , Sandra D Kienast , Rościsław Krutyhołowa , Mikołaj Sokołowski , Urszula Jankowska , Przemysław Grudnik , Sebastian A Leidel , Sebastian Glatt
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Gene Synthesis and CtUrm1 (UniProt ID: G0SE11) were codon-optimized for expression in Escherichia coli, obtained from Genscript Get A Quote

摘要

The chemical modification of tRNA bases by sulfur is crucial to tune translation and to optimize protein synthesis. In eukaryotes, the ubiquitin-related modifier 1 (Urm1) pathway is responsible for the synthesis of 2-thiolated wobble uridine (U34 ). During the key step of the modification cascade, the E1-like activating enzyme ubiquitin-like protein activator 4 (Uba4) first adenylates and thiocarboxylates the C-terminus of its substrate Urm1. Subsequently, activated thiocarboxylated Urm1 (Urm1-COSH) can serve as a sulfur donor for specific tRNA thiolases or participate in ubiquitin-like conjugation reactions. Structural and mechanistic details of Uba4 and Urm1 have remained elusive but are key to understand the... More

关键词

adenylation; tRNA modification; thioester; thiolation; ubiquitin-like proteins. © 2020 The Authors. Published under the terms of the CC BY 4.0 license.