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Structural basis for specific recognition of Lys 63-linked polyubiquitin chains by NZF domains of TAB2 and TAB3

机译:TAB2和TAB3的NZF域特异性识别Lys 63连接的多聚泛素链的结构基础

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摘要

TAB2 and TAB3 activate the Jun N-terminal kinase and nuclear factor-κB pathways through the specific recognition of Lys 63-linked polyubiquitin chains by its Npl4 zinc-finger (NZF) domain. Here we report crystal structures of the TAB2 and TAB3 NZF domains in complex with Lys 63-linked diubiquitin at 1.18 and 1.40 Å resolutions, respectively. Both NZF domains bind to the distal ubiquitin through a conserved Thr-Phe dipeptide that has been shown to be important for the interaction of the NZF domain of Npl4 with monoubiquitin. In contrast, a surface specific to TAB2 and TAB3 binds the proximal ubiquitin. Both the distal and proximal binding sites of the TAB2 and TAB3 NZF domains recognize the Ile 44-centred hydrophobic patch on ubiquitin but do not interact with the Lys 63-linked isopeptide bond. Mutagenesis experiments show that both binding sites are required to enable binding of Lys 63-linked diubiquitin. We therefore propose a mechanism for the recognition of Lys 63-linked polyubiquitin chains by TAB2 and TAB3 NZF domains in which diubiquitin units are specifically recognized by a single NZF domain.
机译:TAB2和TAB3通过其Npl4锌指(NZF)域对Lys 63连接的多聚泛蛋白链的特异性识别,激活了Jun N端激酶和核因子-κB通路。在这里,我们分别以1.18和1.40Å的分辨率报告了与Lys 63连接的双泛素复合的TAB2和TAB3 NZF域的晶体结构。两个NZF结构域均通过保守的Thr-Phe二肽结合至远端遍在蛋白,这对于Npl4的NZF结构域与单遍在蛋白的相互作用是重要的。相反,TAB2和TAB3的特定表面会结合近端泛素。 TAB2和TAB3 NZF域的远端和近端结合位点均识别泛素上以Ile 44为中心的疏水性补丁,但不与Lys 63连接的异肽键相互作用。诱变实验表明,两个结合位点都是使Lys 63连接的双泛素结合所需的。因此,我们提出了一种机制,用于通过TAB2和TAB3 NZF域识别Lys 63-连接的多泛素链,其中双泛素单元被单个NZF域特异性识别。

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