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氙气的镇静作用是通过与表达于小鼠腹侧基底核丘脑皮质神经元的 HCN2 通道的环核苷酸结合域(CNBD)相互作用介导的。

Xenon's Sedative Effect Is Mediated by Interaction with the Cyclic Nucleotide-Binding Domain (CNBD) of HCN2 Channels Expressed by Thalamocortical Neurons of the Ventrobasal Nucleus in Mice.

机构信息

Department of Anesthesiology and Intensive Care Medicine, Klinikum Rechts der Isar, School of Medicine, Technical University of Munich, 81675 Munich, Germany.

Department of Pharmacy-Center for Drug Research, Ludwig-Maximilians-Universitñt Mnchen, 81377 Munich, Germany.

出版信息

Int J Mol Sci. 2023 May 11;24(10):8613. doi: 10.3390/ijms24108613.

Abstract

Previous studies have shown that xenon reduces hyperpolarization-activated cyclic nucleotide-gated channels type-2 (HCN2) channel-mediated current (I) amplitude and shifts the half-maximal activation voltage (V1/2) in thalamocortical circuits of acute brain slices to more hyperpolarized potentials. HCN2 channels are dually gated by the membrane voltage and via cyclic nucleotides binding to the cyclic nucleotide-binding domain (CNBD) on the channel. In this study, we hypothesize that xenon interferes with the HCN2 CNBD to mediate its effect. Using the transgenic mice model HCN2EA, in which the binding of cAMP to HCN2 was abolished by two amino acid mutations (R591E, T592A), we performed ex-vivo patch-clamp recordings and in-vivo open-field test to prove this hypothesis. Our data showed that xenon (1.9 mM) application to brain slices shifts the V1/2 of I to more hyperpolarized potentials in wild-type thalamocortical neurons (TC) (V1/2: -97.09 [-99.56--95.04] mV compared to control -85.67 [-94.47--82.10] mV; = 0.0005). These effects were abolished in HCN2EA neurons (TC), whereby the V1/2 reached only -92.56 [-93.16- -89.68] mV with xenon compared to -90.03 [-98.99--84.59] mV in the control ( = 0.84). After application of a xenon mixture (70% xenon, 30% O), wild-type mice activity in the open-field test decreased to 5 [2-10] while in HCN2EA mice it remained at 30 [15-42]%, ( = 0.0006). In conclusion, we show that xenon impairs HCN2 channel function by interfering with the HCN2 CNBD site and provide in-vivo evidence that this mechanism contributes to xenon-mediated hypnotic properties.

摘要

先前的研究表明,氙气可减少 hyperpolarization-activated cyclic nucleotide-gated channels type-2 (HCN2) 通道介导的电流 (I) 幅度,并将丘脑皮质电路中 HCN2 通道的半激活电压 (V1/2) 向超极化方向移动。HCN2 通道由膜电压和通过与通道上的环核苷酸结合域 (CNBD) 结合的环核苷酸双重门控。在这项研究中,我们假设氙气干扰 HCN2 CNBD 以介导其作用。使用转基因小鼠模型 HCN2EA,其中通过两个氨基酸突变 (R591E、T592A) 消除了 cAMP 与 HCN2 的结合,我们进行了离体膜片钳记录和体内旷场测试来验证这一假设。我们的数据表明,氙气 (1.9 mM) 应用于脑片可使野生型丘脑皮质神经元 (TC) 的 I 的 V1/2 向更超极化的电位移动 (V1/2:-97.09 [-99.56--95.04] mV 与对照相比为 -85.67 [-94.47--82.10] mV;= 0.0005)。这些效应在 HCN2EA 神经元 (TC) 中被消除,其中与对照相比,氙气仅使 V1/2 达到 -92.56 [-93.16- -89.68] mV,为 -90.03 [-98.99--84.59] mV ( = 0.84)。在应用氙气混合物 (70%氙气,30% O) 后,野生型小鼠在旷场测试中的活动减少到 5 [2-10],而在 HCN2EA 小鼠中仍保持在 30 [15-42]%,( = 0.0006)。总之,我们表明氙气通过干扰 HCN2 CNBD 位点来损害 HCN2 通道功能,并提供体内证据表明,这种机制有助于氙气介导的催眠特性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a847/10218445/19457e80aa5a/ijms-24-08613-g001.jpg

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