RING proteins constitute the largest class of E3 ubiquitin ligases. Unlike most RINGs, AO7 (RNF25) binds the E2 ubiquitin-conjugating enzyme, UbcH5B (UBE2D2), with strikingly high affinity. We have defined, by co-crystallization, the distinctive means by which AO7 binds UbcH5B. AO7 contains a structurally unique UbcH5B binding region (U5BR) that is connected by an 11-amino acid linker to its RING domain, forming a clamp surrounding the E2. The U5BR interacts extensively with a region of UbcH5B that is distinct from both the active site and the RING-interacting region, referred to as the backside of the E2. An apparent paradox is that the high-affinity binding of the AO7 clamp to UbcH5B, which is dependent on the U5BR, decreases the rate of ubiquitination. We establish that this is a consequence of blocking the stimulatory, non-covalent, binding of ubiquitin to the backside of UbcH5B. Interestingly, when non-covalent backside ubiquitin binding cannot occur, the AO7 clamp now enhances the rate of ubiquitination. The high-affinity binding of the AO7 clamp to UbcH5B has also allowed for the co-crystallization of previously described and functionally important RING mutants at the RING-E2 interface. We show that mutations having marked effects on function only minimally affect the intermolecular interactions between the AO7 RING and UbcH5B, establishing a high degree of complexity in activation through the RING-E2 interface.
Insights into Ubiquitination from the Unique Clamp-like Binding of the RING E3 AO7 to the E2 UbcH5B.
从 RING E3 AO7 与 E2 UbcH5B 的独特钳状结合中了解泛素化
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作者:Li Shengjian, Liang Yu-He, Mariano Jennifer, Metzger Meredith B, Stringer Daniel K, Hristova Ventzislava A, Li Jess, Randazzo Paul A, Tsai Yien Che, Ji Xinhua, Weissman Allan M
| 期刊: | Journal of Biological Chemistry | 影响因子: | 3.900 |
| 时间: | 2015 | 起止号: | 2015 Dec 18; 290(51):30225-39 |
| doi: | 10.1074/jbc.M115.685867 | 研究方向: | 表观遗传 |
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