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四价铵阻断剂对 TREK-1 通道的细胞内无状态进入。

State-independent intracellular access of quaternary ammonium blockers to the pore of TREK-1.

机构信息

Physiological Institute, Christian-Albrechts University, Kiel, Germany.

出版信息

Channels (Austin). 2012 Nov-Dec;6(6):473-8. doi: 10.4161/chan.22153. Epub 2012 Sep 18.

Abstract

We previously reported that TREK-1 gating by internal pH and pressure occurs close to or within the selectivity filter. These conclusions were based upon kinetic measurements of high-affinity block by quaternary ammonium (QA) ions that appeared to exhibit state-independent accessibility to their binding site within the pore. Intriguingly, recent crystal structures of two related K2P potassium channels were also both found to be open at the helix bundle crossing. However, this did not exclude the possibility of gating at the bundle crossing and it was suggested that side-fenestrations within these structures might allow state-independent access of QA ions to their binding site. In this addendum to our original study we demonstrate that even hydrophobic QA ions do not access the TREK-1 pore via these fenestrations. Furthermore, by using a chemically reactive QA ion immobilized within the pore via covalent cysteine modification we provide additional evidence that the QA binding site remains accessible to the cytoplasm in the closed state. These results support models of K2P channel gating which occur close to or within the selectivity filter and do not involve closure at the helix bundle crossing.

摘要

我们之前曾报道,TREK-1 门控由内部 pH 值和压力引起,发生在选择性过滤器附近或其中。这些结论是基于对高亲和力阻断的动力学测量得出的,这些阻断似乎表现出对其在孔内结合位点的状态独立可及性。有趣的是,最近两个相关的 K2P 钾通道的晶体结构也都被发现处于开放状态在螺旋束交叉处。然而,这并没有排除在束交叉处发生门控的可能性,并有人提出这些结构中的侧窗可能允许 QA 离子对其结合位点进行状态独立的进入。在我们原始研究的这个附录中,我们证明即使是疏水性的 QA 离子也不能通过这些窗孔进入 TREK-1 孔。此外,通过使用通过半胱氨酸共价修饰固定在孔内的反应性 QA 离子,我们提供了额外的证据表明,在关闭状态下,QA 结合位点仍然可及细胞质。这些结果支持 K2P 通道门控模型,这些模型发生在选择性过滤器附近或其中,而不涉及在螺旋束交叉处的关闭。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/730b/3536734/2785dbdbd175/chan-6-473-g1.jpg

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