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钾敏感受体 KdpD 的跨膜 GAF 结构域的结构与功能。

Structure and function of the juxtamembrane GAF domain of potassium biosensor KdpD.

机构信息

Department of Biochemistry, Duke University Medical Center, Durham, North Carolina, USA.

Department of Biological Sciences, Purdue University, West Lafayette, Indiana, USA.

出版信息

Protein Sci. 2020 Sep;29(9):2009-2021. doi: 10.1002/pro.3920. Epub 2020 Aug 17.

Abstract

KdpD/KdpE two-component signaling system regulates expression of a high affinity potassium transporter responsible for potassium homeostasis. The C-terminal module of KdpD consists of a GAF domain linked to a histidine kinase domain. Whereas certain GAF domains act as regulators by binding cyclic nucleotides, the role of the juxtamembrane GAF domain in KdpD is unknown. We report the high-resolution crystal structure of KdpD GAF domain (KdpD ) consisting of five α-helices, four β-sheets and two large loops. KdpD forms a symmetry-related dimer, wherein parallelly arranged monomers contribute to a four-helix bundle at the dimer-interface, SAXS analysis of KdpD C-terminal module reveals an elongated structure that is a dimer in solution. Substitution of conserved residues with various residues that disrupt the dimer interface produce a range of effects on gene expression demonstrating the importance of the interface in inactive to active transitions during signaling. Comparison of ligand binding site of the classic cyclic nucleotide-binding GAF domains to KdpD reveals structural differences arising from naturally occurring substitutions in primary sequence of KdpD that modifies the canonical NKFDE sequence motif required for cyclic nucleotide binding. Together these results suggest a structural role for KdpD in dimerization and transmission of signal to the kinase domain.

摘要

KdpD/KdpE 双组分信号系统调节高亲和钾转运体的表达,该转运体负责钾离子稳态。KdpD 的 C 末端模块由 GAF 结构域与组氨酸激酶结构域相连组成。虽然某些 GAF 结构域通过结合环核苷酸起调节作用,但 KdpD 中膜旁 GAF 结构域的作用尚不清楚。我们报道了 KdpD GAF 结构域(KdpD )的高分辨率晶体结构,该结构域由五个α螺旋、四个β片层和两个大环组成。KdpD 形成对称相关的二聚体,其中平行排列的单体在二聚体界面处贡献一个四螺旋束,KdpD C 末端模块的 SAXS 分析显示出一种在溶液中为二聚体的伸长结构。用各种破坏二聚体界面的保守残基取代产生了一系列对基因表达的影响,证明了界面在信号传递过程中从非活性到活性转变中的重要性。将经典环核苷酸结合 GAF 结构域的配体结合位点与 KdpD 进行比较,揭示了由于 KdpD 一级序列中天然发生的取代而产生的结构差异,这些取代改变了环核苷酸结合所需的典型 NKFDE 序列基序。这些结果共同表明 KdpD 在二聚化和信号向激酶结构域传递中的结构作用。

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