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线粒体钙单向转运蛋白的双环离子选择性过滤器的离子和抑制剂结合。

Ion and inhibitor binding of the double-ring ion selectivity filter of the mitochondrial calcium uniporter.

机构信息

Department of Biological Chemistry and Molecular Pharmacology, Harvard Medical School, Boston, MA 02115.

State Key Laboratory of Elemento-Organic Chemistry, Collaborative Innovation Center of Chemical Science and Engineering (Tianjin), Nankai University, Tianjin 300071, China.

出版信息

Proc Natl Acad Sci U S A. 2017 Apr 4;114(14):E2846-E2851. doi: 10.1073/pnas.1620316114. Epub 2017 Mar 21.

Abstract

The calcium (Ca) uniporter of mitochondria is a holocomplex consisting of the Ca-conducting channel, known as mitochondrial calcium uniporter (MCU), and several accessory and regulatory components. A previous electrophysiology study found that the uniporter has high Ca selectivity and conductance and this depends critically on the conserved amino acid sequence motif, DXXE (Asp-X-X-Glu) of MCU. A recent NMR structure of the MCU channel from revealed that the DXXE forms two parallel carboxylate rings at the channel entrance that seem to serve as the ion selectivity filter, although direct ion interaction of this structural motif has not been addressed. Here, we use a paramagnetic probe, manganese (Mn), to investigate ion and inhibitor binding of this putative selectivity filter. Our paramagnetic NMR data show that mutants with a single carboxylate ring, NXXE (Asn-X-X-Glu) and DXXQ (Asp-X-X-Gln), each can bind Mn specifically, whereas in the WT the two rings bind Mn cooperatively, resulting in ∼1,000-fold higher apparent affinity. Ca can specifically displace the bound Mn at the DXXE site in the channel. Furthermore, titrating the sample with the known channel inhibitor ruthenium 360 (Ru360) can displace Mn binding from the solvent-accessible Asp site but not the inner Glu site. The NMR titration data, together with structural analysis of the DXXE motif and molecular dynamics simulation, indicate that the double carboxylate rings at the apex of the MCU pore constitute the ion selectivity filter and that Ru360 directly blocks ion entry into the filter by binding to the outer carboxylate ring.

摘要

线粒体的钙(Ca)单通道是一个由钙通道组成的全复合物,称为线粒体钙单通道(MCU),以及几个辅助和调节成分。以前的电生理学研究发现,单通道具有高 Ca 选择性和电导率,这取决于 MCU 的保守氨基酸序列基序 DXXE(天冬氨酸-XX-谷氨酸)。最近的一项 NMR 结构研究揭示了 MCU 通道的结构,该结构表明 DXXE 在通道入口处形成两个平行的羧酸盐环,似乎充当离子选择性过滤器,尽管尚未解决该结构基序的直接离子相互作用。在这里,我们使用顺磁探针锰(Mn)来研究这个假定的选择性过滤器的离子和抑制剂结合。我们的顺磁 NMR 数据表明,具有单个羧酸盐环的突变体 NXXE(Asn-X-X-Glu)和 DXXQ(Asp-X-X-Gln)都可以特异性地结合 Mn,而在 WT 中,两个环协同结合 Mn,导致表观亲和力提高约 1000 倍。Ca 可以特异性地置换通道中 DXXE 位点结合的 Mn。此外,用已知的通道抑制剂钌 360(Ru360)滴定样品可以从溶剂可及的 Asp 位点置换 Mn 结合,但不能从内部 Glu 位点置换。NMR 滴定数据,结合 DXXE 基序的结构分析和分子动力学模拟,表明 MCU 孔顶端的双羧酸盐环构成了离子选择性过滤器,而 Ru360 通过与外羧酸盐环结合直接阻止离子进入过滤器。

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