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HECT E3 UBR5 形成 K48 连接的泛素链的结构快照。

Structural snapshots along K48-linked ubiquitin chain formation by the HECT E3 UBR5.

机构信息

Department of Chemistry, School of Natural Sciences, Technical University of Munich, Garching, Germany.

Department of Molecular Machines and Signaling, Max Planck Institute of Biochemistry, Martinsried, Germany.

出版信息

Nat Chem Biol. 2024 Feb;20(2):190-200. doi: 10.1038/s41589-023-01414-2. Epub 2023 Aug 24.

Abstract

Ubiquitin (Ub) chain formation by homologous to E6AP C-terminus (HECT)-family E3 ligases regulates vast biology, yet the structural mechanisms remain unknown. We used chemistry and cryo-electron microscopy (cryo-EM) to visualize stable mimics of the intermediates along K48-linked Ub chain formation by the human E3, UBR5. The structural data reveal a ≈ 620 kDa UBR5 dimer as the functional unit, comprising a scaffold with flexibly tethered Ub-associated (UBA) domains, and elaborately arranged HECT domains. Chains are forged by a UBA domain capturing an acceptor Ub, with its K48 lured into the active site by numerous interactions between the acceptor Ub, manifold UBR5 elements and the donor Ub. The cryo-EM reconstructions allow defining conserved HECT domain conformations catalyzing Ub transfer from E2 to E3 and from E3. Our data show how a full-length E3, ubiquitins to be adjoined, E2 and intermediary products guide a feed-forward HECT domain conformational cycle establishing a highly efficient, broadly targeting, K48-linked Ub chain forging machine.

摘要

泛素(Ub)链由同源 E6AP C 末端(HECT)家族 E3 连接酶形成,调节着广泛的生物学过程,但结构机制仍不清楚。我们使用化学和冷冻电镜(cryo-EM)来可视化人类 E3、UBR5 形成 K48 连接 Ub 链过程中的稳定中间产物模拟物。结构数据揭示了一个 ≈ 620 kDa 的 UBR5 二聚体作为功能单元,包含一个带有灵活连接的 Ub 相关(UBA)结构域的支架,以及精心排列的 HECT 结构域。通过 UBA 结构域捕获接受 Ub 来形成链,其 K48 被接受 Ub、多种 UBR5 元件和供体 Ub 之间的无数相互作用吸引到活性位点。冷冻电镜重建允许定义保守的 HECT 结构域构象,催化 Ub 从 E2 转移到 E3 和从 E3 转移。我们的数据表明,全长 E3、要连接的泛素、E2 和中间产物如何指导一个前馈 HECT 结构域构象循环,建立一个高效、广泛靶向、K48 连接的 Ub 链形成机器。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e6ae/10830417/fe5923a6758e/41589_2023_1414_Fig1_HTML.jpg

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