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对 Kindlin-3 的生物物理分析揭示了其伸展构象,并将整合素结合到膜远端β亚基 NPXY 基序上进行了定位。

Biophysical analysis of Kindlin-3 reveals an elongated conformation and maps integrin binding to the membrane-distal β-subunit NPXY motif.

机构信息

Division of Structural Biology, Wellcome Trust Centre for Human Genetics, Roosevelt Drive, University of Oxford, Oxford OX3 7BN, United Kingdom.

出版信息

J Biol Chem. 2012 Nov 2;287(45):37715-31. doi: 10.1074/jbc.M112.415208. Epub 2012 Sep 18.

DOI:10.1074/jbc.M112.415208
PMID:22989875
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3488048/
Abstract

Kindlin-3, a 75-kDa protein, has been shown to be critical for hemostasis, immunity, and bone metabolism via its role in integrin activation. The Kindlin family is hallmarked by a FERM domain comprised of F1, F2, and F3 subdomains together with an N-terminal F0 domain and a pleckstrin homology domain inserted in the F2 domain. Recombinant Kindlin-3 was cloned, expressed, and purified, and its domain organization was studied by x-ray scattering and other techniques to reveal an extended conformation. This unusual elongated structure is similar to that found in the paralogue Talin head domain. Analytical ultracentrifugation experiments indicated that Kindlin-3 forms a ternary complex with the Talin and β-integrin cytoplasmic tails. NMR showed that Kindlin-3 specifically recognizes the membrane-distal tail NPXY motif in both the β(1A) and β(1D) isoforms, although the interaction is stronger with β(1A). An upstream Ser/Thr cluster in the tails also plays a critical role. Overall these data support current biological, clinical, and mutational data on Kindlin-3/β-tail binding and provide novel insights into the overall conformation and interactions of Kindlin-3.

摘要

Kindlin-3 是一种 75kDa 的蛋白质,通过其在整合素激活中的作用,对于止血、免疫和骨代谢至关重要。Kindlin 家族的特点是 FERM 结构域,由 F1、F2 和 F3 亚结构域以及 N 端 F0 结构域和插入 F2 结构域的 pleckstrin 同源结构域组成。克隆、表达和纯化了重组 Kindlin-3,并通过 X 射线散射和其他技术研究了其结构域组织,揭示了一种扩展构象。这种不寻常的细长结构类似于其同源物 Talin 头部结构域的结构。分析超速离心实验表明,Kindlin-3 与 Talin 和 β 整合素胞质尾部形成三元复合物。NMR 表明,Kindlin-3 特异性识别 β(1A)和 β(1D)同工型中膜远端尾部 NPXY 基序,尽管与 β(1A)的相互作用更强。尾部中的上游 Ser/Thr 簇也起着关键作用。总的来说,这些数据支持了当前关于 Kindlin-3/β-尾结合的生物学、临床和突变数据,并为 Kindlin-3 的整体构象和相互作用提供了新的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0a32/3488048/f3f259591446/zbc0471229240011.jpg
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