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HCN编码的起搏器通道:从生理与生物物理学到生物工程学

HCN-encoded pacemaker channels: from physiology and biophysics to bioengineering.

作者信息

Siu C-W, Lieu D K, Li R A

机构信息

Stem Cell Program, University of California, Davis, CA 95817, USA.

出版信息

J Membr Biol. 2006;214(3):115-22. doi: 10.1007/s00232-006-0881-9. Epub 2007 Jun 8.

Abstract

The depolarizing membrane ionic current I(h) (also known as I(f), "f" for funny), encoded by the hyperpolarization-activated cyclic-nucleotide-modulated (HCN1-4) channel gene family, was first discovered in the heart over 25 years ago. Later, I(h) was also found in neurons, retina, and taste buds. HCN channels structurally resemble voltage-gated K(+) (Kv) channels but the molecular features underlying their opposite gating behaviors (activation by hyperpolarization rather than depolarization) and non-selective permeation profiles (> or =25 times less selective for K(+) than Kv channels) remain largely unknown. Although I(h) has been functionally linked to biological processes from the autonomous beating of the heart to pain transmission, the underlying mechanistic actions remain largely inferential and, indeed, somewhat controversial due to the slow kinetics and negative operating voltage range relative to those of the bioelectrical events involved (e.g., cardiac pacing). This article reviews the current state of our knowledge in the structure-function properties of HCN channels in the context of their physiological functions and potential HCN-based therapies via bioengineering.

摘要

去极化膜离子电流I(h)(也称为I(f),“f”代表“奇特”)由超极化激活的环核苷酸调节(HCN1 - 4)通道基因家族编码,25多年前首次在心脏中被发现。后来,I(h)也在神经元、视网膜和味蕾中被发现。HCN通道在结构上类似于电压门控钾离子(Kv)通道,但它们相反的门控行为(由超极化而非去极化激活)和非选择性渗透特性(对钾离子的选择性比Kv通道低25倍或更多)背后的分子特征在很大程度上仍然未知。尽管I(h)在从心脏自主跳动到疼痛传递等生物过程中都有功能联系,但其潜在的作用机制在很大程度上仍然是推测性的,并且由于其相对于所涉及的生物电事件(如心脏起搏)而言动力学缓慢且工作电压范围为负,实际上存在一定争议。本文在HCN通道的生理功能以及通过生物工程基于HCN的潜在治疗方法的背景下,综述了我们目前对HCN通道结构 - 功能特性的认识状况。

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