Citations to this article

Molecular identification of the role of voltage-gated K+ channels, Kv1.5 and Kv2.1, in hypoxic pulmonary vasoconstriction and control of resting membrane potential in rat pulmonary artery myocytes.
S L Archer, … , H L Reeve, V Hampl
S L Archer, … , H L Reeve, V Hampl
Published June 1, 1998
Citation Information: J Clin Invest. 1998;101(11):2319-2330. https://doi.org/10.1172/JCI333.
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Research Article

Molecular identification of the role of voltage-gated K+ channels, Kv1.5 and Kv2.1, in hypoxic pulmonary vasoconstriction and control of resting membrane potential in rat pulmonary artery myocytes.

Abstract

Hypoxia initiates pulmonary vasoconstriction (HPV) by inhibiting one or more voltage-gated potassium channels (Kv) in the pulmonary artery smooth muscle cells (PASMCs) of resistance arteries. The resulting membrane depolarization increases opening of voltage-gated calcium channels, raising cytosolic Ca2+ and initiating HPV. There are presently nine families of Kv channels known and pharmacological inhibitors lack the specificity to distinguish those involved in control of resting membrane potential (Em) or HPV. However, the Kv channels involved in Em and HPV have characteristic electrophysiological and pharmacological properties which suggest their molecular identity. They are slowly inactivating, delayed rectifier currents, inhibited by 4-aminopyridine (4-AP) but insensitive to charybdotoxin. Candidate Kv channels with these traits (Kv1.5 and Kv2.1) were studied. Antibodies were used to immunolocalize and functionally characterize the contribution of Kv1. 5 and Kv2.1 to PASMC electrophysiology and vascular tone. Immunoblotting confirmed the presence of Kv1.1, 1.2, 1.3, 1.5, 1.6, and 2.1, but not Kv1.4, in PASMCs. Intracellular administration of anti-Kv2.1 inhibited whole cell K+ current (IK) and depolarized Em. Anti-Kv2.1 also elevated resting tension and diminished 4-AP-induced vasoconstriction in membrane-permeabilized pulmonary artery rings. Anti-Kv1.5 inhibited IK and selectively reduced the rise in [Ca2+]i and constriction caused by hypoxia and 4-AP. However, anti-Kv1.5 neither caused depolarization nor elevated basal pulmonary artery tone. This study demonstrates that antibodies can be used to dissect the whole cell K+ currents in mammalian cells. We conclude that Kv2. 1 is an important determinant of resting Em in PASMCs from resistance arteries. Both Kv2.1 and Kv1.5 contribute to the initiation of HPV.

Authors

S L Archer, E Souil, A T Dinh-Xuan, B Schremmer, J C Mercier, A El Yaagoubi, L Nguyen-Huu, H L Reeve, V Hampl

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N Leblanc, AS Forrest, RJ Ayon, M Wiwchar, JE Angermann, HA Pritchard, CA Singer, ML Valencik, F Britton, IA Greenwood 		Pulmonary circulation 2015
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M Pérez-Verdaguer, J Capera, C Serrano-Novillo, I Estadella, D Sastre, A Felipe 		Expert Opinion on Therapeutic Targets 2015
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J Yu, MH Park, SH Jo 		European Journal of Pharmacology 2015
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F Veit, O Pak, RP Brandes, N Weissmann 		Antioxidants & Redox Signaling 2015
Tanshinone IIA attenuates hypoxic pulmonary hypertension via modulating KV currents
L Zheng, M Liu, M Wei, Y Liu, M Dong, Y Luo, P Zhao, H Dong, W Niu, Z Yan, Z Li 		Respiratory Physiology & Neurobiology 2015
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ZK Dai, YW Liu, JH Hsu, JL Yeh, IJ Chen, JR Wu, BN Wu 		International journal of biological sciences 2015
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Ning Lai, Wenju Lu, Jian Wang 		International journal of clinical and experimental pathology 2015
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Ning Lai, Wenju Lu, Jian Wang 		International journal of clinical and experimental pathology 2015
THE INHIBITORY EFFECT OF PACLITAXEL ON (KV2.1) K+ CURRENT IN H9c2 CELLS
N Kitamura, K Sakamoto, T Ono, J Kimura 		FUKUSHIMA JOURNAL OF MEDICAL SCIENCE 2015
Modulation of Closed−State Inactivation in Kv2.1/Kv6.4 Heterotetramers as Mechanism for 4−AP Induced Potentiation
JI Stas, E Bocksteins, AJ Labro, DJ Snyders, AG Obukhov 		PloS one 2015
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