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NMR 揭示了 Stam2 VHS 结构域与泛素和二聚泛素结合的不同模式。

NMR reveals a different mode of binding of the Stam2 VHS domain to ubiquitin and diubiquitin.

机构信息

Université de Lyon, UMR-CNRS 5180 Sciences Analytiques, 69622 Villeurbanne, France.

出版信息

Biochemistry. 2011 Jan 11;50(1):48-62. doi: 10.1021/bi101594a. Epub 2010 Dec 13.

Abstract

The VHS domain of the Stam2 protein is a ubiquitin binding domain involved in the recognition of ubiquitinated proteins committed to lysosomal degradation. Among all VHS domains, the VHS domain of Stam proteins is the strongest binder to monoubiqiuitin and exhibits preferences for K63-linked chains. In the present paper, we report the solution NMR structure of the Stam2-VHS domain in complex with monoubiquitin by means of chemical shift perturbations, spin relaxation, and paramagnetic relaxation enhancements. We also characterize the interaction of Stam2-VHS with K48- and K63-linked diubiquitin chains and report the first evidence that VHS binds differently to these two chains. Our data reveal that VHS enters the hydrophobic pocket of K48-linked diubiquitin and binds the two ubiquitin subunits with different affinities. In contrast, VHS interacts with K63-linked diubiquitin in a mode similar to its interaction with monoubiquitin. We also suggest possible structural models for both K48- and K63-linked diubiquitin in interaction with VHS. Our results, which demonstrate a different mode of binding of VHS for K48- and K63-linked diubiquitin, may explain the preference of VHS for K63- over K48-linked diubiquitin chains and monoubiquitin.

摘要

Stam2 蛋白的 VHS 结构域是一个泛素结合结构域,参与识别将要被溶酶体降解的泛素化蛋白质。在所有的 VHS 结构域中,Stam 蛋白的 VHS 结构域与单泛素的结合能力最强,并且对 K63 连接的链具有偏好性。在本论文中,我们通过化学位移扰动、自旋弛豫和顺磁弛豫增强等方法,报道了 Stam2-VHS 结构域与单泛素复合物的溶液 NMR 结构。我们还研究了 Stam2-VHS 与 K48 和 K63 连接的二泛素链的相互作用,并首次证明了 VHS 与这两种链的结合方式不同。我们的数据表明,VHS 进入 K48 连接的二泛素的疏水性口袋,并以不同的亲和力结合两个泛素亚基。相比之下,VHS 与 K63 连接的二泛素以类似于与单泛素相互作用的方式相互作用。我们还提出了 VHS 与 K48 和 K63 连接的二泛素相互作用的可能结构模型。我们的结果表明,VHS 对 K48 和 K63 连接的二泛素的结合方式不同,这可能解释了 VHS 对 K63 连接的二泛素链和单泛素的偏好性。

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