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钙通道γ6亚基是低电压激活(Cav3.1)钙电流的独特调节剂。

Calcium channel gamma6 subunits are unique modulators of low voltage-activated (Cav3.1) calcium current.

作者信息

Hansen Jared P, Chen Ren-Shiang, Larsen Janice K, Chu Po-Ju, Janes Donna M, Weis Karen E, Best Philip M

机构信息

Department of Molecular and Integrative Physiology, University of Illinois at Urbana-Champaign, 524 Burrill Hall, MC-114, 407 S. Goodwin Avenue, Urbana, IL 61801, USA.

出版信息

J Mol Cell Cardiol. 2004 Dec;37(6):1147-58. doi: 10.1016/j.yjmcc.2004.08.005.

Abstract

The calcium channel gamma (gamma) subunit family consists of eight members whose functions include modulation of high voltage-activated (HVA) calcium currents in skeletal muscle and neurons, and regulation of alpha-amino-3-hydroxy-5-methylisoxazole-4-propanoic acid (AMPA) receptor targeting. Cardiac myocytes express at least three gamma subunits, gamma(4), gamma(6) and gamma(7), whose function(s) in the heart are unknown. Here we compare the effects of the previously uncharacterized gamma(6) subunit with that of gamma(4) and gamma(7) on a low voltage-activated calcium channel (Cav3.1) that is expressed in cardiac myocytes. Co-expression of both the long and short gamma(6) subunit isoforms, gamma(6L) and gamma(6S), with Cav3.1 in HEK-293 cells significantly decreases current density by 49% and 69%, respectively. Two other gamma subunits expressed in cardiac myocytes, gamma(4) and gamma(7), have no significant effect on Cav3.1 current. Neither gamma(6L), gamma(6S), gamma(4) nor gamma(7) significantly affect the voltage dependency of activation or inactivation or the kinetics of Cav3.1 current. Transient expression of gamma(6L) in an immortalized atrial cell line (HL-1) significantly reduces the endogenous low voltage-activated current in these cells by 63%. Green fluorescent protein tagged gamma(6L) is localized primarily in HEK-293 cell surface membranes where it is evenly distributed. Expression of gamma(6L) does not affect the level of Cav3.1 mRNA or the amount of total Cav3.1 protein in transfected HEK-293 cells. These results demonstrate that the gamma(6) subunit has a unique ability to inhibit Cav3.1 dependent calcium current that is not shared with the gamma(4) and gamma(7) isoforms and is thus a potential regulator of cardiac low voltage-activated calcium current.

摘要

钙通道γ亚基家族由八个成员组成,其功能包括调节骨骼肌和神经元中的高电压激活(HVA)钙电流,以及调节α-氨基-3-羟基-5-甲基异恶唑-4-丙酸(AMPA)受体靶向。心肌细胞表达至少三种γ亚基,γ(4)、γ(6)和γ(7),它们在心脏中的功能尚不清楚。在这里,我们比较了此前未被表征的γ(6)亚基与γ(4)和γ(7)亚基对心肌细胞中表达的低电压激活钙通道(Cav3.1)的影响。在HEK-293细胞中,长和短γ(6)亚基异构体γ(6L)和γ(6S)与Cav3.1共表达,分别使电流密度显著降低49%和69%。心肌细胞中表达的另外两种γ亚基γ(4)和γ(7)对Cav3.1电流没有显著影响。γ(6L)、γ(6S)、γ(4)和γ(7)均未显著影响Cav3.1电流的激活或失活电压依赖性或动力学。γ(6L)在永生化心房细胞系(HL-1)中的瞬时表达使这些细胞中的内源性低电压激活电流显著降低63%。绿色荧光蛋白标记的γ(6L)主要定位于HEK-293细胞表面膜,且分布均匀。γ(6L)的表达不影响转染的HEK-293细胞中Cav3.1 mRNA的水平或总Cav3.1蛋白的量。这些结果表明,γ(6)亚基具有独特的能力来抑制Cav3.1依赖性钙电流,这是γ(4)和γ(7)异构体所不具备的,因此是心脏低电压激活钙电流的潜在调节因子。

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