Computational Study on Effect of KCNQ1 P535T Mutation in a Cardiac Ventricular Tissue.

IF 2.3 4区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Helan Satish, Ramasubba Reddy Machireddy
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引用次数: 0

Abstract

Heart diseases such as arrhythmia are the main causes of sudden death. Arrhythmias are typically caused by mutations in specific genes, damage in the cardiac tissue, or due to some chemical exposure. Arrhythmias caused due to mutation is called inherited arrhythmia. Induced arrhythmias are caused due to tissue damage or chemical exposure. Mutations in genes that encode ion channels of the cardiac cells usually result in (dysfunction) improper functioning of the channel. Improper functioning of the ion channel may lead to major changes in the action potential (AP) of the cardiac cells. This further leads to distorted electrical activity of the heart. Distorted electrical activity will affect the ECG that results in arrhythmia. KCNQ1 P535T mutation is one such gene mutation that encodes the potassium ion channel (KV7.1) of the cardiac ventricular tissue. Its clinical significance is not known. This study aims to perform a simulation study on P535T mutation in the KCNQ1 gene that encodes the potassium ion channel KV7.1 in the ventricular tissue grid. The effect of P535T mutation on transmural tissue grids for three genotypes (wild type, heterozygous, and homozygous) of cells are studied and the generated pseudo-ECGs are compared. Results show the delayed repolarization in the cells of ventricular tissue grid. Slower propagation of action potential in the transmural tissue grid is observed in the mutated (heterozygous and homozygous) genotypes. Longer QT interval is also observed in the pseudo-ECG of heterozygous and homozygous genotype tissue grids. From the pseudo-ECGs, it is observed that KCNQ1 P535T mutation leads to Long QT Syndrome (LQTS) which may result in life-threatening arrhythmias, such as Torsade de Pointes (TdP), Jervell and Lange-Nielsen syndrome (JLNS), and Romano-Ward syndrome (RWS).

Abstract Image

KCNQ1 P535T突变对心脏心室组织影响的计算研究
心律失常等心脏疾病是导致猝死的主要原因。心律失常通常是由特定基因的突变、心脏组织的损伤或某些化学物质暴露引起的。由基因突变引起的心律失常称为遗传性心律失常。诱发性心律失常是由于组织损伤或化学物质暴露引起的。心肌细胞离子通道编码基因的突变通常会导致离子通道功能不正常。离子通道功能不正常可导致心肌细胞动作电位(AP)发生重大变化。这进一步导致了心脏电活动的扭曲。扭曲的电活动将影响心电图,导致心律失常。KCNQ1 P535T突变就是其中一种编码心脏心室组织钾离子通道(KV7.1)的基因突变。其临床意义尚不清楚。本研究旨在对编码心室组织网格钾离子通道KV7.1的KCNQ1基因P535T突变进行模拟研究。研究了P535T突变对三种基因型(野生型、杂合型和纯合型)细胞跨壁组织网格的影响,并比较了产生的伪心电图。结果表明,脑室组织网格细胞存在延迟复极现象。在突变(杂合和纯合)基因型中观察到跨壁组织网格中动作电位的缓慢传播。杂合子和纯合子基因型组织网格的伪心电图QT间期也较长。伪心电图显示,KCNQ1 P535T突变可导致长QT综合征(LQTS), LQTS可导致危及生命的心律失常,如Torsade de Pointes (TdP)、Jervell and lge - nielsen综合征(JLNS)、Romano-Ward综合征(RWS)。
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来源期刊
Journal of Membrane Biology
Journal of Membrane Biology 生物-生化与分子生物学
CiteScore
4.80
自引率
4.20%
发文量
63
审稿时长
6-12 weeks
期刊介绍: The Journal of Membrane Biology is dedicated to publishing high-quality science related to membrane biology, biochemistry and biophysics. In particular, we welcome work that uses modern experimental or computational methods including but not limited to those with microscopy, diffraction, NMR, computer simulations, or biochemistry aimed at membrane associated or membrane embedded proteins or model membrane systems. These methods might be applied to study topics like membrane protein structure and function, membrane mediated or controlled signaling mechanisms, cell-cell communication via gap junctions, the behavior of proteins and lipids based on monolayer or bilayer systems, or genetic and regulatory mechanisms controlling membrane function. Research articles, short communications and reviews are all welcome. We also encourage authors to consider publishing ''negative'' results where experiments or simulations were well performed, but resulted in unusual or unexpected outcomes without obvious explanations. While we welcome connections to clinical studies, submissions that are primarily clinical in nature or that fail to make connections to the basic science issues of membrane structure, chemistry and function, are not appropriate for the journal. In a similar way, studies that are primarily descriptive and narratives of assays in a clinical or population study are best published in other journals. If you are not certain, it is entirely appropriate to write to us to inquire if your study is a good fit for the journal.
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