Abstract

The long-term objective of our research is to understand how cardiac ion channels are modulated by pharmacological agents and by pathological conditions. This information is critical for the design of efficacious antiarrhythmic agents and effective management of cardiac arrhythmias under pathological conditions. The key to achieving this objective is to have a thorough understanding of the structure-function relationship of cardiac ion channels. The advance of molecular cloning and mutagenesis techniques has allowed us to correlate cloned channel subunits with native channels in the heart, and to manipulate their primary sequences in specific ways so that the relation between channel structure and function can be deduced. The focus of this application is the rapid (IKr) and slow (IKs) delayed rectifier K channels in the heart. IKr and IKs are the primary determinants of action potential duration (APD) in cardiac myocytes. Their importance in maintaining the normal cardiac electrical activity is related to their unique gating properties. The fast inactivation and reactivation processes of IKr cause an inward rectification in its I-V. This helps maintain a positive plateau phase during phase 2 and yet sufficient outward current for phase 3 repolarization. On the other hand, the slow activation and deactivation processes of IKs are an important mechanism for APD regulation by changes in the heart rate. These slow gating processes are related to the interactions between two subunits of IKs: KvLQT1 and hIsK. IKr and IKs are also important targets for K channel modulators. Information about the mechanisms and sites of actions of currently available K channel modulators on IKr and IKs may aid the design of new antiarrhythmic drugs. We propose to use cloned K channel subunits as a model (hERG for IKr and KvLQT1/hIsK for IKs), and combine site- directed mutagenesis and electrophysiological techniques to study the structure-function relationship and drug-channel interactions.
Four Specific Aims are proposed: (1) To study the structural basis for the unique gating behavior of hERG, (2) To study the mechanisms of azimilide s agonist and antagonist actions on hERG, (3) To study the domains of KvLQT1 involved in interactions with hIsK, (4) To study the mechanisms of differential actions of azimilide and quinidine on IKs. It is anticipated that results from these studies will improve our understanding of the function and modulation of IKr and IKs, and the studies on azimilide and quinidine should provide far-reaching implications for drug actions on K channels.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
2R01HL046451-04A1
Application #
2632990
Study Section
Cardiovascular and Pulmonary Research A Study Section (CVA)
Project Start
1994-06-01
Project End
2002-03-31
Budget Start
1998-04-01
Budget End
1999-03-31
Support Year
4
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Columbia University (N.Y.)
Department
Pharmacology
Type
Schools of Medicine
DUNS #
167204994
City
New York
State
NY
Country
United States
Zip Code
10032

  Publications

Jiang, Min; Xu, Xulin; Wang, Yuhong et al. (2009) Dynamic partnership between KCNQ1 and KCNE1 and influence on cardiac IKs current amplitude by KCNE2. J Biol Chem 284:16452-62
Xu, Xulin; Jiang, Min; Hsu, Kai-Ling et al. (2008) KCNQ1 and KCNE1 in the IKs channel complex make state-dependent contacts in their extracellular domains. J Gen Physiol 131:589-603
Xu, Xulin; Recanatini, Maurizio; Roberti, Marinella et al. (2008) Probing the binding sites and mechanisms of action of two human ether-a-go-go-related gene channel activators, 1,3-bis-(2-hydroxy-5-trifluoromethyl-phenyl)-urea (NS1643) and 2-[2-(3,4-dichloro-phenyl)-2,3-dihydro-1H-isoindol-5-ylamino]-nicotinic acid (PD3 Mol Pharmacol 73:1709-21
Tseng, Gea-Ny (2007) The phenotype of a KCNQ1 mutation depends on its KCNE partners: is the cardiac slow delayed rectifier (IKs) channel more than a KCNQ1/KCNE1 complex? Heart Rhythm 4:1542-3
Tseng, Gea-Ny; Sonawane, Kailas D; Korolkova, Yuliya V et al. (2007) Probing the outer mouth structure of the HERG channel with peptide toxin footprinting and molecular modeling. Biophys J 92:3524-40
Liu, Xian-Sheng; Zhang, Mei; Jiang, Min et al. (2007) Probing the interaction between KCNE2 and KCNQ1 in their transmembrane regions. J Membr Biol 216:117-27
Zhang, M; Liu, X-S; Diochot, S et al. (2007) APETx1 from sea anemone Anthopleura elegantissima is a gating modifier peptide toxin of the human ether-a-go-go- related potassium channel. Mol Pharmacol 72:259-68
Wu, Dong-Mei; Jiang, Min; Zhang, Mei et al. (2006) KCNE2 is colocalized with KCNQ1 and KCNE1 in cardiac myocytes and may function as a negative modulator of I(Ks) current amplitude in the heart. Heart Rhythm 3:1469-80
Wu, Dong-Mei; Lai, Ling-Ping; Zhang, Mei et al. (2006) Characterization of an LQT5-related mutation in KCNE1, Y81C: implications for a role of KCNE1 cytoplasmic domain in IKs channel function. Heart Rhythm 3:1031-40
Zhang, M; Liu, J; Jiang, M et al. (2005) Interactions between charged residues in the transmembrane segments of the voltage-sensing domain in the hERG channel. J Membr Biol 207:169-81

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