Vandenberg, Jamie I and Perry, Matthew D and Perrin, Mark J and Mann, Stefan A and Ke, Ying and Hill, Adam P (2012) hERG K(+) channels: structure, function, and clinical significance. Physiological reviews, 92 (3). pp. 1393-478. ISSN 1522-1210 (OA)
Vandenberg, Jamie I and Perry, Matthew D and Perrin, Mark J and Mann, Stefan A and Ke, Ying and Hill, Adam P (2012) hERG K(+) channels: structure, function, and clinical significance. Physiological reviews, 92 (3). pp. 1393-478. ISSN 1522-1210 (OA)
Vandenberg, Jamie I and Perry, Matthew D and Perrin, Mark J and Mann, Stefan A and Ke, Ying and Hill, Adam P (2012) hERG K(+) channels: structure, function, and clinical significance. Physiological reviews, 92 (3). pp. 1393-478. ISSN 1522-1210 (OA)
Abstract
The human ether-a-go-go related gene (hERG) encodes the pore-forming subunit of the rapid component of the delayed rectifier K(+) channel, Kv11.1, which are expressed in the heart, various brain regions, smooth muscle cells, endocrine cells, and a wide range of tumor cell lines. However, it is the role that Kv11.1 channels play in the heart that has been best characterized, for two main reasons. First, it is the gene product involved in chromosome 7-associated long QT syndrome (LQTS), an inherited disorder associated with a markedly increased risk of ventricular arrhythmias and sudden cardiac death. Second, blockade of Kv11.1, by a wide range of prescription medications, causes drug-induced QT prolongation with an increase in risk of sudden cardiac arrest. In the first part of this review, the properties of Kv11.1 channels, including biogenesis, trafficking, gating, and pharmacology are discussed, while the second part focuses on the pathophysiology of Kv11.1 channels. (NHMRC grants 459401, 1019693; ARC grant FT110100075; National Heart Foundation of Australia, and the St Vincent's Clinic Foundation).
Metadata
Subjects: | R Medicine > R Medicine (General) |
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Depositing User: | Ms Britt Granath |
Date Deposited: | 21 Dec 2015 02:29 |
Last Modified: | 22 Jan 2016 03:07 |