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人心脏T型Ca2+通道基因家族成员alpha1H的克隆与特性分析

Cloning and characterization of alpha1H from human heart, a member of the T-type Ca2+ channel gene family.

作者信息

Cribbs L L, Lee J H, Yang J, Satin J, Zhang Y, Daud A, Barclay J, Williamson M P, Fox M, Rees M, Perez-Reyes E

机构信息

Department of Physiology, Cardiovascular Institute, Loyola University Medical Center, Maywood, Ill 60153, USA.

出版信息

Circ Res. 1998 Jul 13;83(1):103-9. doi: 10.1161/01.res.83.1.103.

DOI:10.1161/01.res.83.1.103
PMID:9670923
Abstract

Voltage-activated Ca2+ channels exist as multigene families that share common structural features. Different Ca2+ channels are distinguished by their electrophysiology and pharmacology and can be classified as either low or high voltage-activated channels. Six alpha1 subunit genes cloned previously code for high voltage-activated Ca2+ channels; therefore, we have used a database search strategy to identify new Ca2+ channel genes, possibly including low voltage-activated (T-type) channels. A novel expressed sequence-tagged cDNA clone of alpha1G was used to screen a cDNA library, and in the present study, we report the cloning of alpha1H (or CavT.2), a low voltage-activated Ca2+ channel from human heart. Northern blots of human mRNA detected more alpha1H expression in peripheral tissues, such as kidney and heart, than in brain. We mapped the gene, CACNA1H, to human chromosome 16p13.3 and mouse chromosome 17. Expression of alpha1H in HEK-293 cells resulted in Ca2+ channel currents displaying voltage dependence, kinetics, and unitary conductance characteristic of native T-type Ca2+ channels. The alpha1H channel is sensitive to mibefradil, a nondihydropyridine Ca2+ channel blocker, with an IC50 of 1.4 micromol/L, consistent with the reported potency of mibefradil for T-type Ca2+ channels. Together with alpha1G, a rat brain T-type Ca2+ channel also cloned in our laboratory, these genes define a unique family of Ca2+ channels.

摘要

电压门控性Ca2+通道以具有共同结构特征的多基因家族形式存在。不同的Ca2+通道可通过其电生理学和药理学特性加以区分,可分为低电压激活通道或高电压激活通道。先前克隆的6个α1亚基基因编码高电压激活的Ca2+通道;因此,我们采用数据库搜索策略来鉴定新的Ca2+通道基因,可能包括低电压激活(T型)通道。利用一个新的α1G表达序列标签cDNA克隆筛选cDNA文库,在本研究中,我们报告了从人心脏克隆出的低电压激活Ca2+通道α1H(或CavT.2)。人mRNA的Northern印迹显示,外周组织如肾脏和心脏中α1H的表达比脑中更多。我们将该基因CACNA1H定位于人染色体16p13.3和小鼠染色体17。α1H在HEK-293细胞中的表达导致Ca2+通道电流呈现出天然T型Ca2+通道的电压依赖性、动力学和单位电导特性。α1H通道对非二氢吡啶类Ca2+通道阻滞剂米贝地尔敏感,IC50为1.4 μmol/L,这与报道的米贝地尔对T型Ca2+通道的效力一致。与我们实验室也克隆出的大鼠脑T型Ca2+通道α1G一起,这些基因定义了一个独特的Ca2+通道家族。

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