2015
DOI: 10.1016/j.molcel.2015.02.017
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Activation of a Primed RING E3-E2–Ubiquitin Complex by Non-Covalent Ubiquitin

Abstract: RING ubiquitin ligases (E3) recruit ubiquitin-conjugate enzymes (E2) charged with ubiquitin (Ub) to catalyze ubiquitination. Non-covalent Ub binding to the backside of certain E2s promotes processive polyUb formation, but the mechanism remains elusive. Here, we show that backside bound Ub (Ub(B)) enhances both RING-independent and RING-dependent UbcH5B-catalyzed donor Ub (Ub(D)) transfer, but with a more prominent effect in RING-dependent transfer. Ub(B) enhances RING E3s' affinities for UbcH5B-Ub, and RING E3… Show more

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Cited by 118 publications
(192 citation statements)
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“…Through structural and mutagenesis studies, we identify a novel and conserved mechanism through which canonical PCGF2/4 limits the activity of RING1. In addition, we demonstrate that, contrary to expectation 6,30 , PCGF-RING1 ligases use a mode of Ub recognition and activation 31 highly similar to that recently discovered for homodimeric RING E3s 30,32,33 and monomeric RINGs CBL-B and RNF38 34,35 . In contrast to the differences in their intrinsic catalytic activities, we find all the six PCGF-RING1 heterodimers to be robust H2A ligases in an assay using purified components.…”
supporting
confidence: 64%
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“…Through structural and mutagenesis studies, we identify a novel and conserved mechanism through which canonical PCGF2/4 limits the activity of RING1. In addition, we demonstrate that, contrary to expectation 6,30 , PCGF-RING1 ligases use a mode of Ub recognition and activation 31 highly similar to that recently discovered for homodimeric RING E3s 30,32,33 and monomeric RINGs CBL-B and RNF38 34,35 . In contrast to the differences in their intrinsic catalytic activities, we find all the six PCGF-RING1 heterodimers to be robust H2A ligases in an assay using purified components.…”
supporting
confidence: 64%
“…Structures of RING E3s in complex with charged UbcH5-family E2s reveal a consistent arrangement of the E2, the RING and Ub 30,31,[33][34][35] ( Fig. 3; Supplementary Fig.…”
Section: Models Of E3-e2bub Complexes Suggest a Basis For Activationmentioning
confidence: 86%
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“…Other than at the E2 active site, ubiquitin also binds to a specific region on the "backside" of a subset of E2s (Ub B binding), which enhances RING:E2 affinity and stimulates ubiquitination (17)(18)(19)(20). Several E3s also bind their cognate E2s on secondary sites away from the RING-E2 interface.…”
mentioning
confidence: 99%