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非成孔β亚基在电压门控钠通道生理和病理生理中的作用。

The role of non-pore-forming β subunits in physiology and pathophysiology of voltage-gated sodium channels.

作者信息

Calhoun Jeffrey D, Isom Lori L

机构信息

Department of Pharmacology, University of Michigan, Ann Arbor, MI, 48109-5632, USA.

出版信息

Handb Exp Pharmacol. 2014;221:51-89. doi: 10.1007/978-3-642-41588-3_4.

Abstract

Voltage-gated sodium channel β1 and β2 subunits were discovered as auxiliary proteins that co-purify with pore-forming α subunits in brain. The other family members, β1B, β3, and β4, were identified by homology and shown to modulate sodium current in heterologous systems. Work over the past 2 decades, however, has provided strong evidence that these proteins are not simply ancillary ion channel subunits, but are multifunctional signaling proteins in their own right, playing both conducting (channel modulatory) and nonconducting roles in cell signaling. Here, we discuss evidence that sodium channel β subunits not only regulate sodium channel function and localization but also modulate voltage-gated potassium channels. In their nonconducting roles, VGSC β subunits function as immunoglobulin superfamily cell adhesion molecules that modulate brain development by influencing cell proliferation and migration, axon outgrowth, axonal fasciculation, and neuronal pathfinding. Mutations in genes encoding β subunits are linked to paroxysmal diseases including epilepsy, cardiac arrhythmia, and sudden infant death syndrome. Finally, β subunits may be targets for the future development of novel therapeutics.

摘要

电压门控钠通道β1和β2亚基最初是作为与脑中形成孔道的α亚基共同纯化的辅助蛋白被发现的。其他家族成员β1B、β3和β4则是通过同源性鉴定出来的,并已证明它们能在异源系统中调节钠电流。然而,过去20年的研究提供了强有力的证据,表明这些蛋白质并非仅仅是辅助性离子通道亚基,而是本身就具有多功能的信号蛋白,在细胞信号传导中发挥传导(通道调节)和非传导作用。在此,我们讨论有关钠通道β亚基不仅调节钠通道功能和定位,还能调节电压门控钾通道的证据。在其非传导作用中,电压门控钠通道β亚基作为免疫球蛋白超家族细胞粘附分子发挥作用,通过影响细胞增殖和迁移、轴突生长、轴突成束以及神经元路径寻找来调节脑发育。编码β亚基的基因突变与包括癫痫、心律失常和婴儿猝死综合征在内的阵发性疾病有关。最后,β亚基可能是新型治疗药物未来开发的靶点。

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