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Structural and functional analysis of a talin triple domain module suggests an alternative talin autoinhibitory configuration

机译:塔林三重结构域模块的结构和功能分析表明塔林具有自身抑制作用

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摘要

Talin plays important role in regulating integrin-mediated signaling. Talin function is autoinhibited by intramolecular interactions between the integrin-binding F3 domain and the autoinhibitory domain (R9). We determined the crystal structure of a triple domain fragment R7R8R9, which contains R9 and the RIAM (Rap1-Interacting Adaptor Molecule) binding domain (R8). The structure reveals a crystallographic contact between R9 and a symmetrically related R8 domain, representing a homodimeric interaction in talin. Strikingly, we demonstrated that the α5 helix of R9 also interacts with the F3 domain, despite no interdomain contact involving the α5 helix in the crystal structure of an F2F3:R9 autoinhibitory complex reported previously. Mutations on the α5 helix significantly diminish the F3:R9 association and lead to elevated talin activity. Our results offer the biochemical and functional evidence of the existence of a new talin autoinhibitory configuration, thus providing a more comprehensive understanding of talin autoinhibition, regulation, and quaternary structure assembly.
机译:塔林在调节整联蛋白介导的信号传导中起重要作用。通过整合素结合的F3结构域和自抑制域(R9)之间的分子内相互作用,塔林功能被自抑制。我们确定了一个三结构域片段R7R8R9的晶体结构,该片段包含R9和RIAM(Rap1-相互作用衔接分子)结合域(R8)。该结构揭示了R9与对称相关R8域之间的晶体学接触,代表塔林中的同二聚体相互作用。令人惊讶地,我们证明了R9的α5螺旋也与F3域相互作用,尽管先前报道的F2F3:R9自抑制复合物的晶体结构中没有涉及α5螺旋的域间接触。 α5螺旋上的突变显着降低了F3:R9缔合并导致塔林活性升高。我们的结果提供了新的talin自动抑制构型的存在的生化和功能证据,从而提供了talin自动抑制,调节和四级结构组装的更全面的了解。

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