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Role of the amino and carboxy termini in isoform-specific sodium channel variation

机译:氨基和羧基末端在亚型特异性钠通道变异中的作用

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摘要

Nav1.2 and Nav1.6 are two voltage-gated sodium channel isoforms found in adult CNS neurons. These isoforms differ in their electrophysiological properties, even though the major regions that are known to be involved in channel activation and inactivation are conserved between them. To determine if the terminal domains of these channels contributed to their activation and fast inactivation differences, we constructed chimeras between the two isoforms and characterized their electrophysiological properties. Exchanging the N-terminal 205 amino acids of Nav1.6 and the corresponding 202 amino acids of Nav1.2 completely swapped the V_1/2 of steady-state activation between the Nav1.2 and Nav1.6 channels in an isoform-specific manner. Exchanging the C-terminal 436 amino acids of Nav1.6 and the corresponding region of Nav1.2 altered the voltage dependence and kinetics of steady-state inactivation, but the changes did not reflect a direct transfer of inactivation properties between the two isoforms. Finally, the N- and C-terminal domains from Nav1.6 demonstrated functional cooperation. These results suggest that the terminal sequences of the sodium channel are important for isoform-specific differences between the channels.
机译:Nav1.2和Nav1.6是在成人CNS神经元中发现的两种电压门控钠通道亚型。这些同工型在电生理特性上有所不同,即使已知在通道激活和失活中涉及的主要区域在它们之间是保守的。为了确定这些通道的末端结构域是否有助于其激活和快速失活的差异,我们在两个同工型之间构建了嵌合体,并表征了它们的电生理特性。交换Nav1.6的N端205个氨基酸和Nav1.2的对应202个氨基酸,可以在Nav1.2和Nav1.6之间完全交换稳态激活的V_ 1 / 2通道以异构体特异性方式表达。交换Nav1.6的C末端436个氨基酸和Nav1.2的相应区域改变了电压依赖性和稳态灭活的动力学,但这些变化并未反映出两种同工型之间灭活特性的直接转移。最后,来自Nav1.6的N和C末端域证明了功能上的合作。这些结果表明,钠通道的末端序列对于通道之间的同工型特异性差异很重要。

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