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首页> 外文期刊>Nature Communications >Legionella effector MavC targets the Ube2N~Ub conjugate for noncanonical ubiquitination
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Legionella effector MavC targets the Ube2N~Ub conjugate for noncanonical ubiquitination

机译:军团菌效应器MAVC针对非甘露苷ubiquitination的UBE2N〜UB缀合物

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摘要

The bacterial effector MavC modulates the host immune response by blocking Ube2N activity employing an E1-independent ubiquitin ligation, catalyzing formation of a γ-glutamyl-ε-Lys (Gln40 Ub -Lys92 Ube2N ) isopeptide crosslink using a transglutaminase mechanism. Here we provide biochemical evidence in support of MavC targeting the activated, thioester-linked Ube2N~ubiquitin conjugate, catalyzing an intramolecular transglutamination reaction, covalently crosslinking the Ube2N and Ub subunits effectively inactivating the E2~Ub conjugate. Ubiquitin exhibits weak binding to MavC alone, but shows an increase in affinity when tethered to Ube2N in a disulfide-linked substrate that mimics the charged E2~Ub conjugate. Crystal structures of MavC in complex with the substrate mimic and crosslinked product provide insights into the reaction mechanism and underlying protein dynamics that favor transamidation over deamidation, while revealing a crucial role for the structurally unique insertion domain in substrate recognition. This work provides a structural basis of ubiquitination by transglutamination and identifies this enzyme's true physiological substrate.
机译:细菌效应子MAVC通过阻断ube2N活性来调节宿主免疫应答,所述ube2n活性使用γ-谷氨酸-ε-lys(Gln40 Ub -lys92ube2n)使用转谷氨酰胺酶机构催化形成γ-谷氨酸-ε-lys(gln40ub -lys92ube2n)。在这里,我们提供生物化学证据,以支持MAVC靶向活化的硫酯连接的UBE2N〜ubiquitin缀合物,催化分子内转谷氨酸反应,共价交联,有效地将E2〜UB缀合物灭活e2〜UB缀合物。泛素单独表现出与MAVC的弱结合,但显示在二硫化物连接的基底中与UBE2N系在模拟电荷的E2〜UB缀合物中时的亲和力的增加。 MAVC的晶体结构与基材模拟和交联产物的综合性提供了进入反应机制的洞察力和有利于脱染的副作用的底层蛋白质动态,同时揭示基底识别中结构独特的插入结构域的至关重要作用。该工作通过转谷酰胺提供泛素化的结构基础,并鉴定该酶的真正生理基质。

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