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- W1981111452 startingPage "1833" @default.
- W1981111452 abstract "Post-translational protein modifications initiate, regulate, propagate and terminate a wide variety of processes in cells, and in particular, ubiquitylation targets substrate proteins for degradation, subcellular translocation, cell signaling and multiple other cellular events. Modification of substrate proteins is widely observed to occur via covalent linkages of ubiquitin to the amine groups of lysine side-chains. However, in recent years several new modes of ubiquitin chain attachment have emerged. For instance, covalent modification of non-lysine sites in substrate proteins is theoretically possible according to basic chemical principles underlying the ubiquitylation process, and evidence is building that sites such as the N-terminal amine group of a protein, the hydroxyl group of serine and threonine residues and even the thiol groups of cysteine residues are all employed as sites of ubiquitylation. However, the potential importance of this “non-canonical ubiquitylation” of substrate proteins on sites other than lysine residues has been largely overlooked. This review aims to highlight the unusual features of the process of non-canonical ubiquitylation and the consequences of these events on the activity and fate of a protein." @default.
- W1981111452 created "2016-06-24" @default.
- W1981111452 creator A5029833703 @default.
- W1981111452 creator A5066636121 @default.
- W1981111452 date "2013-08-01" @default.
- W1981111452 modified "2023-10-12" @default.
- W1981111452 title "Non-canonical ubiquitylation: Mechanisms and consequences" @default.
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- W1981111452 doi "https://doi.org/10.1016/j.biocel.2013.05.026" @default.