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双侧阻断双拓扑F通道。

Two-sided block of a dual-topology F- channel.

作者信息

Turman Daniel L, Nathanson Jacob T, Stockbridge Randy B, Street Timothy O, Miller Christopher

机构信息

Department of Biochemistry and Howard Hughes Medical Institute, Brandeis University, Waltham, MA 02454.

Department of Biochemistry and.

出版信息

Proc Natl Acad Sci U S A. 2015 May 5;112(18):5697-701. doi: 10.1073/pnas.1505301112. Epub 2015 Apr 20.

Abstract

The Fluc family is a set of small membrane proteins forming F(-)-specific electrodiffusive ion channels that rescue microorganisms from F(-) toxicity during exposure to weakly acidic environments. The functional channel is built as a dual-topology homodimer with twofold symmetry parallel to the membrane plane. Fluc channels are blocked by nanomolar-affinity fibronectin-domain monobodies originally selected from phage-display libraries. The unusual symmetrical antiparallel dimeric architecture of Flucs demands that the two chemically equivalent monobody-binding epitopes reside on opposite ends of the channel, a double-sided blocking situation that has never before presented itself in ion channel biophysics. However, it is not known if both sites can be simultaneously occupied, and if so, whether monobodies bind independently or cooperatively to their transmembrane epitopes. Here, we use direct monobody-binding assays and single-channel recordings of a Fluc channel homolog to reveal a novel trimolecular blocking behavior that reveals a doubly occupied blocked state. Kinetic analysis of single-channel recordings made with monobody on both sides of the membrane shows substantial negative cooperativity between the two blocking sites.

摘要

Fluc家族是一组小的膜蛋白,它们形成F(-)特异性电扩散离子通道,在暴露于弱酸性环境时能使微生物免受F(-)毒性影响。功能性通道构建为具有与膜平面平行的二重对称性的双拓扑同型二聚体。Fluc通道被最初从噬菌体展示文库中筛选出的具有纳摩尔亲和力的纤连蛋白结构域单克隆抗体所阻断。Flucs这种不寻常的对称反平行二聚体结构要求两个化学等价的单克隆抗体结合表位位于通道的相对两端,这种双面阻断情况在离子通道生物物理学中从未出现过。然而,尚不清楚两个位点是否能同时被占据,如果可以,单克隆抗体是独立还是协同结合到它们的跨膜表位上。在这里,我们使用直接的单克隆抗体结合测定和Fluc通道同源物的单通道记录来揭示一种新的三分子阻断行为,该行为揭示了一种双重占据的阻断状态。对在膜两侧使用单克隆抗体进行的单通道记录的动力学分析表明,两个阻断位点之间存在显著的负协同作用。

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Proof of dual-topology architecture of Fluc F- channels with monobody blockers.
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