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磷酸肌醇调节双孔通道 3 第二个重复中的 S4 电压传感器的动态运动。

Phosphoinositide regulates dynamic movement of the S4 voltage sensor in the second repeat in two-pore channel 3.

机构信息

Division of Biophysics and Neurobiology, National Institute for Physiological Sciences, Okazaki, Japan; Department of Physiological Sciences, The Graduate University for Advanced Studies, Hayama, Japan.

Division of Biophysics and Neurobiology, National Institute for Physiological Sciences, Okazaki, Japan; Department of Physiological Sciences, The Graduate University for Advanced Studies, Hayama, Japan.

出版信息

J Biol Chem. 2021 Dec;297(6):101425. doi: 10.1016/j.jbc.2021.101425. Epub 2021 Nov 18.

Abstract

The two-pore channels (TPCs) are voltage-gated cation channels consisting of single polypeptides with two repeats of a canonical 6-transmembrane unit. TPCs are known to be regulated by various physiological signals such as membrane voltage and phosphoinositide (PI). The fourth helix in the second repeat (second S4) plays a major role in detecting membrane voltage, whereas the first repeat contains a PI binding site. Therefore, each of these stimuli is detected by a unique repeat to regulate the gating of the TPC central pore. How these various stimuli regulate the dynamic structural rearrangement of the TPC molecule remain unknown. Here, we found that PI binding to the first repeat in TPC3 regulates the movement of the distally located second S4 helix, showing that the PI-binding signal is not confined to the pore gate but also transmitted to the voltage sensor. Using voltage clamp fluorometry, measurement of gating charges, and Cys-accessibility analysis, we observed that PI binding significantly potentiates the voltage dependence of the movement of the second S4 helix. Notably, voltage clamp fluorometry analysis revealed that the voltage-dependent movement of the second S4 helix occurred in two phases, of which the second phase corresponds to the transfer of the gating charges. This movement was observed in the voltage range where gate-opening occurs and was potentiated by PI. In conclusion, this regulation of the second S4 helix by PI indicates a tight inter-repeat coupling within TPC3, a feature which might be conserved among TPC family members to integrate various physiological signals.

摘要

双孔通道(TPCs)是由单一多肽组成的电压门控阳离子通道,具有两个重复的经典 6 跨膜单元。已知 TPCs 受多种生理信号调节,如膜电压和磷酸肌醇(PI)。第二个重复的第四个螺旋(第二个 S4)在检测膜电压方面起着主要作用,而第一个重复包含一个 PI 结合位点。因此,这些刺激中的每一种都通过独特的重复来检测,以调节 TPC 中央孔的门控。这些不同的刺激如何调节 TPC 分子的动态结构重排仍然未知。在这里,我们发现 PI 与 TPC3 中的第一个重复结合调节远端第二 S4 螺旋的运动,表明 PI 结合信号不仅局限于孔门,而且还传递到电压传感器。使用电压钳荧光法、门控电荷测量和 Cys 可及性分析,我们观察到 PI 结合显著增强了第二 S4 螺旋运动对电压的依赖性。值得注意的是,电压钳荧光法分析表明,第二 S4 螺旋的电压依赖性运动发生在两个阶段,其中第二阶段对应于门控电荷的转移。这种运动发生在门控打开的电压范围内,并且被 PI 增强。总之,PI 对第二 S4 螺旋的这种调节表明 TPC3 中重复之间的紧密相互作用,这一特征可能在 TPC 家族成员中保守,以整合各种生理信号。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/51db/8665364/d88aec24a5ed/gr1.jpg

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