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合成的Shaker球肽对大电导钙激活钾通道的状态依赖性阻断

State-dependent block of BK channels by synthesized shaker ball peptides.

作者信息

Li Weiyan, Aldrich Richard W

机构信息

Section of Neurobiology, University of Texas at Austin, Austin, TX 78712, USA.

出版信息

J Gen Physiol. 2006 Oct;128(4):423-41. doi: 10.1085/jgp.200609521. Epub 2006 Sep 11.

Abstract

Crystal structures of potassium channels have strongly corroborated an earlier hypothetical picture based on functional studies, in which the channel gate was located on the cytoplasmic side of the pore. However, accessibility studies on several types of ligand-sensitive K(+) channels have suggested that their activation gates may be located near or within the selectivity filter instead. It remains to be determined to what extent the physical location of the gate is conserved across the large K(+) channel family. Direct evidence about the location of the gate in large conductance calcium-activated K(+) (BK) channels, which are gated by both voltage and ligand (calcium), has been scarce. Our earlier kinetic measurements of the block of BK channels by internal quaternary ammonium ions have raised the possibility that they may lack a cytoplasmic gate. We show in this study that a synthesized Shaker ball peptide (ShBP) homologue acts as a state-dependent blocker for BK channels when applied internally, suggesting a widening at the intracellular end of the channel pore upon gating. This is consistent with a gating-related conformational change at the cytoplasmic end of the pore-lining helices, as suggested by previous functional and structural studies on other K(+) channels. Furthermore, our results from two BK channel mutations demonstrate that similar types of interactions between ball peptides and channels are shared by BK and other K(+) channel types.

摘要

钾通道的晶体结构有力地证实了基于功能研究的早期假设图景,即通道门位于孔道的胞质侧。然而,对几种类型的配体敏感性钾通道的可及性研究表明,它们的激活门可能位于选择性过滤器附近或内部。门的物理位置在整个大的钾通道家族中保守的程度仍有待确定。关于大电导钙激活钾(BK)通道门位置的直接证据一直很少,BK通道由电压和配体(钙)共同门控。我们早期对内部季铵离子阻断BK通道的动力学测量提出了它们可能缺乏胞质门的可能性。我们在这项研究中表明,一种合成的Shaker球肽(ShBP)同源物在内部应用时可作为BK通道的状态依赖性阻断剂,表明门控时通道孔的细胞内端变宽。这与孔道内衬螺旋的胞质端与门控相关的构象变化一致,正如先前对其他钾通道的功能和结构研究所表明的那样。此外,我们对两个BK通道突变的研究结果表明,球肽与通道之间的类似相互作用类型在BK和其他钾通道类型中是共有的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fc4e/2151574/d523e25a1ae0/jgp1280423f01.jpg

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