Pharmacology of the short QT syndrome N588K-hERG K+ channel mutation: differential impact on selected class I and class III antiarrhythmic drugs

机译：短QT综合征N588K-hERG K +通道突变的药理作用：对所选的I类和III类抗心律不齐药物的差异影响

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Background and purpose:The short QT syndrome (SQTS) is associated with cardiac arrhythmias and sudden death. The SQT1 form of SQTS results from an inactivation-attenuated, gain-of-function mutation (N588K) to the human ether-à-go-go-related gene (hERG) potassium channel. Pharmacological blockade of this mutated hERG channel may have therapeutic value. However, hERG-blocking potencies of canonical inhibitors such as E-4031 and D-sotalol are significantly reduced for N588K-hERG. Here, five hERG-blocking drugs were compared to determine their relative potencies for inhibiting N588K channels, and two other inactivation-attenuated mutant channels were tested to investigate the association between impaired inactivation and altered drug potency.

机译：背景与目的：短QT综合征（SQTS）与心律不齐和猝死有关。 SQT1的SQT1形式是由与人类随身携带相关基因（hERG）钾通道失活而减弱的功能获得性突变（N588K）产生的。该突变的hERG通道的药理学阻断作用可能具有治疗价值。但是，对于N588K-hERG，规范抑制剂（例如E-4031和D-索他洛尔）的hERG阻断能力显着降低。在这里，比较了五种hERG阻滞药物，以确定它们抑制N588K通道的相对效能，并测试了另外两个失活衰减的突变体通道，以研究失活的受损与改变的药物效能之间的关系。

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期刊名称 British Journal of Pharmacology and Chemotherapy
作者
M J McPate; R S Duncan; J C Hancox; H J Witchel;
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作者单位

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年(卷),期 2008(155),6
年度 2008
页码 957–966
总页数 10
原文格式 PDF
正文语种
中图分类药学;
关键词
hERG human ether-à-go-go-related gene IKr inactivation KCNH2 KV11.1 N588K QT interval rapid delayed rectifier potassium current short QT syndrome SQTS;

机译：hERG;与人在一起的醚相关基因;IKr;失活;KCNH2;KV11.1;N588K;QT间隔;快速延迟整流钾电流;短QT综合征;SQTS;

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1. Vascular effects of class-III antiarrhythmic drugs: chromanol 293B, but not dofetilide blocks the smooth muscle delayed rectifier K+ channel. [J] . Karle CA, Bauer A, Weretka S, Basic Research in Cardiology: Official Journal of the German Association of Cardiovascular Research . 2002,第1期

机译：Ⅲ类抗心律不齐药物的血管作用：苯并二氢吡喃二甲酚293B，但非多美利特没有阻断平滑肌延迟的整流器K +通道。
2. Inhibition of I_(K,ACh) current may contribute to clinical efficacy of class I and class III antiarrhythmic drugs in patients with atrial fibrillationNiels Voi Nadiia Rozmaritsa; Anne Trausch; Thomasz Zimniak; Torsten Christ; Erich Wettwer; Klaus Matschke; Dobromir Dobrev; Ursula RavensDepartment of Pharmacology and Toxicology, Dresden University of Technology, Fetscherstr. 74, 01307 Dresden, Germany [J] . Naunyn-Schmiedeberg's Archives of Pharmacology . 2010,第3期

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3. Effects of landiolol, an ultra-short-acting beta1-selective blocker, on electrical storm refractory to class III antiarrhythmic drugs. [J] . Miwa Y, Ikeda T, Mera H, Circulation journal . 2010,第5期

机译：兰诺洛尔（一种超短效β1选择性阻滞剂）对难治III级抗心律不齐药物的电风暴的影响。
4. In silico investigation of short QT syndrome-linked potassium channel mutations on electro-mechanical function of human atrial cells [C] . Dominic G Whittaker, Michael A Colman, Haibo Ni, Computing in Cardiology Conference . 2015

机译：短QT综合征相关的钾通道突变对人心房细胞机电功能的计算机分析
5. Functional analysis of hERG potassium channels and mutations underlying the Long QT Syndrome. [D] . Saenen, Johan B. 2007

机译：hERG钾通道和长QT综合征基础突变的功能分析。
6. Effects of class III antiarrhythmic drugs on the Na(+)-activated K+ channels in guinea-pig ventricular cells. [O] . K. Mori, T. Saito, Y. Masuda, 1996

机译：III类抗心律不齐药物对豚鼠心室细胞Na（+）激活的K +通道的影响。
7. Pharmacology of the short QT syndrome N588K-hERG K+ channel mutation: differential impact on selected class I and class III antiarrhythmic drugs [O] . McPate, M J, Duncan, R S, Hancox, J C, 2008

机译：短QT综合征N588K-hERG K +通道突变的药理作用：对所选的I类和III类抗心律不齐药物的差异影响

Pharmacology of the short QT syndrome N588K-hERG K+ channel mutation: differential impact on selected class I and class III antiarrhythmic drugs

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