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可溶性鸟苷酸环化酶刺激剂 IWP-051 存在和不存在条件下希瓦氏菌 H-NOX 蛋白的溶液结构。

Solution structures of the Shewanella woodyi H-NOX protein in the presence and absence of soluble guanylyl cyclase stimulator IWP-051.

机构信息

Department of Chemistry and Biochemistry, University of Arizona, Tucson, Arizona, USA.

National Magnetic Resonance Facility at Madison, Biochemistry Department, University of Wisconsin-Madison, Madison, Wisconsin, USA.

出版信息

Protein Sci. 2021 Feb;30(2):448-463. doi: 10.1002/pro.4005. Epub 2020 Dec 10.

DOI:10.1002/pro.4005
PMID:33236796
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7784750/
Abstract

Heme-nitric oxide/oxygen binding (H-NOX) domains bind gaseous ligands for signal transduction in organisms spanning prokaryotic and eukaryotic kingdoms. In the bioluminescent marine bacterium Shewanella woodyi (Sw), H-NOX proteins regulate quorum sensing and biofilm formation. In higher animals, soluble guanylyl cyclase (sGC) binds nitric oxide with an H-NOX domain to induce cyclase activity and regulate vascular tone, wound healing and memory formation. sGC also binds stimulator compounds targeting cardiovascular disease. The molecular details of stimulator binding to sGC remain obscure but involve a binding pocket near an interface between H-NOX and coiled-coil domains. Here, we report the full NMR structure for CO-ligated Sw H-NOX in the presence and absence of stimulator compound IWP-051, and its backbone dynamics. Nonplanar heme geometry was retained using a semi-empirical quantum potential energy approach. Although IWP-051 binding is weak, a single binding conformation was found at the interface of the two H-NOX subdomains, near but not overlapping with sites identified in sGC. Binding leads to rotation of the subdomains and closure of the binding pocket. Backbone dynamics are similar across both domains except for two helix-connecting loops, which display increased dynamics that are further enhanced by compound binding. Structure-based sequence analyses indicate high sequence diversity in the binding pocket, but the pocket itself appears conserved among H-NOX proteins. The largest dynamical loop lies at the interface between Sw H-NOX and its binding partner as well as in the interface with the coiled coil in sGC, suggesting a critical role for the loop in signal transduction.

摘要

血红素-一氧化氮/氧结合(H-NOX)结构域结合气态配体,在跨越原核生物和真核生物王国的生物体中进行信号转导。在发光海洋细菌希瓦氏菌(Sw)中,H-NOX 蛋白调节群体感应和生物膜形成。在高等动物中,可溶性鸟苷酸环化酶(sGC)通过 H-NOX 结构域结合一氧化氮,诱导环化酶活性并调节血管张力、伤口愈合和记忆形成。sGC 还结合针对心血管疾病的刺激化合物。刺激物与 sGC 结合的分子细节仍然不清楚,但涉及到 H-NOX 和卷曲螺旋结构域之间界面附近的结合口袋。在这里,我们报道了 CO 结合的 Sw H-NOX 在存在和不存在刺激化合物 IWP-051 时的完整 NMR 结构及其骨架动力学。使用半经验量子势能方法保留了非平面血红素几何形状。尽管 IWP-051 结合较弱,但在两个 H-NOX 亚结构域的界面处发现了一个单一的结合构象,位于 sGC 中确定的位点附近但不重叠。结合导致亚结构域旋转和结合口袋关闭。除了两个连接螺旋的环外,两个结构域的骨架动力学相似,这些环的动力学增加,化合物结合进一步增强。基于结构的序列分析表明,结合口袋中的序列多样性很高,但口袋本身在 H-NOX 蛋白中似乎是保守的。最大的动态环位于 Sw H-NOX 与其结合伙伴之间的界面以及 sGC 中与卷曲螺旋的界面上,表明该环在信号转导中起着关键作用。

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