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首页> 外文期刊>Heart rhythm: the official journal of the Heart Rhythm Society >A pore-localizing CACNA1C-E1115K missense mutation, identified in a patient with idiopathic QT prolongation, bradycardia, and autism spectrum disorder, converts the L-type calcium channel into a hybrid nonselective monovalent cation channel
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A pore-localizing CACNA1C-E1115K missense mutation, identified in a patient with idiopathic QT prolongation, bradycardia, and autism spectrum disorder, converts the L-type calcium channel into a hybrid nonselective monovalent cation channel

机译:一个pore-localizing CACNA1C-E1115K错义突变,特发性患者确认QT延长、心动过缓和自闭症障碍,将l型钙通道成一个混合非选择性单价阳离子通道

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摘要

BACKGROUND Gain-of-function variants in the CACNA1C-encoded L-type calcium channel (LTCC, Ca(v)1.2) cause type 8 long QT syndrome (LQT8). The pore region contains highly conserved glutamic acid (E) residues that collectively form the LTCC's selectivity filter. Here, we identified and characterized a pore-localizing missense variant, E1115K, that yielded a novel perturbation in the LTCC.
机译:后台功能变体CACNA1C-encoded l型钙通道高瓦斯,Ca (v) 1.2)导致8型长QT综合征(LQT8)。孔区域包含高度保守的谷氨酸(E)共同形成的残留物确立的选择性过滤器。pore-localizing识别和特征E1115K错义变异,产生了一部小说在确立扰动。

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