Biophysical mechanisms of myocardium sodium channelopathies.

IF 2.9 4区 医学 Q2 PHYSIOLOGY Pflugers Archiv : European journal of physiology Pub Date : 2024-05-01 Epub Date: 2024-03-01 DOI:10.1007/s00424-024-02930-3
Anastasia K Zaytseva, Olga E Kulichik, Anna A Kostareva, Boris S Zhorov
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Abstract

Genetic variants of gene SCN5A encoding the alpha-subunit of cardiac voltage-gated sodium channel Nav1.5 are associated with various diseases, including long QT syndrome (LQT3), Brugada syndrome (BrS1), and progressive cardiac conduction disease (PCCD). In the last decades, the great progress in understanding molecular and biophysical mechanisms of these diseases has been achieved. The LQT3 syndrome is associated with gain-of-function of sodium channels Nav1.5 due to impaired inactivation, enhanced activation, accelerated recovery from inactivation or the late current appearance. In contrast, BrS1 and PCCD are associated with the Nav1.5 loss-of-function, which in electrophysiological experiments can be manifested as reduced current density, enhanced fast or slow inactivation, impaired activation, or decelerated recovery from inactivation. Genetic variants associated with congenital arrhythmias can also disturb interactions of the Nav1.5 channel with different proteins or drugs and cause unexpected reactions to drug administration. Furthermore, mutations can affect post-translational modifications of the channels and their sensitivity to pH and temperature. Here we briefly review the current knowledge on biophysical mechanisms of LQT3, BrS1 and PCCD. We focus on limitations of studies that use heterologous expression systems and induced pluripotent stem cells (iPSC) derived cardiac myocytes and summarize our understanding of genotype-phenotype relations of SCN5A mutations.

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心肌钠通道疾病的生物物理机制
编码心脏电压门控钠通道α-亚基 Nav1.5 的基因 SCN5A 的遗传变异与多种疾病相关,包括长 QT 综合征(LQT3)、布鲁格达综合征(BrS1)和进行性心脏传导疾病(PCCD)。在过去几十年中,人们在了解这些疾病的分子和生物物理机制方面取得了重大进展。LQT3 综合征与钠通道 Nav1.5 的功能增益有关,其原因包括失活受损、激活增强、失活恢复加速或电流出现过晚。相比之下,BrS1 和 PCCD 与 Nav1.5 功能缺失有关,在电生理实验中可表现为电流密度降低、快速或慢速失活增强、激活受损或失活恢复减慢。与先天性心律失常相关的基因变异也会扰乱 Nav1.5 通道与不同蛋白质或药物的相互作用,并导致意外的用药反应。此外,基因突变还会影响通道的翻译后修饰及其对 pH 值和温度的敏感性。在此,我们简要回顾了目前有关 LQT3、BrS1 和 PCCD 生物物理机制的知识。我们重点讨论了使用异源表达系统和诱导多能干细胞(iPSC)衍生心肌细胞进行研究的局限性,并总结了我们对 SCN5A 突变的基因型与表型关系的理解。
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来源期刊
CiteScore
8.80
自引率
2.20%
发文量
121
审稿时长
4-8 weeks
期刊介绍: Pflügers Archiv European Journal of Physiology publishes those results of original research that are seen as advancing the physiological sciences, especially those providing mechanistic insights into physiological functions at the molecular and cellular level, and clearly conveying a physiological message. Submissions are encouraged that deal with the evaluation of molecular and cellular mechanisms of disease, ideally resulting in translational research. Purely descriptive papers covering applied physiology or clinical papers will be excluded. Papers on methodological topics will be considered if they contribute to the development of novel tools for further investigation of (patho)physiological mechanisms.
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