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Heteromeric assembly of Kv2.1 with Kv9.3: effect on the state dependence of inactivation.

机译:Kv2.1与Kv9.3的异体组装:对失活状态依赖性的影响。

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摘要

Modulatory alpha-subunits of Kv channels remain electrically silent after homomeric expression. Their interactions with Kv2 alpha-subunits via the amino-terminal domain promote the assembly of heteromeric functional channels. The kinetic features of these heteromers differ from those of Kv2 homomers, suggesting a distinct role in electrical signaling. This study investigates biophysical properties of channels emerging from the coexpression of Kv2.1 with the modulatory alpha-subunit Kv9.3. Changes relative to homomeric Kv2.1 concern activation, deactivation, inactivation, and recovery from inactivation. A detailed description of Kv2.1/Kv9.3 inactivation is presented. Kv2.1/Kv9.3 heteromers inactivate in a fast and complete fashion from intermediate closed states, but in a slow and incomplete manner from open states. Intermediate closed states of channel gating can be approached through partial activation or deactivation, according to a proposed qualitative model. These transitions are rate-limiting for Kv2.1/Kv9.3 inactivation. Finally, based on the kinetic description, we propose a putative function for Kv2.1/Kv9.3 heteromers in rat heart.
机译:同源表达后,Kv通道的调节性α-亚基保持电沉默。它们通过氨基末端结构域与Kv2α-亚基的相互作用促进了异源功能通道的组装。这些杂聚物的动力学特征不同于Kv2同聚物的动力学特征,表明在电信号传导中具有独特的作用。这项研究调查了Kv2.1与调节性α亚基Kv9.3共表达产生的通道的生物物理特性。相对于同型Kv2.1的变化涉及激活,失活,失活以及从失活中恢复。给出了Kv2.1 / Kv9.3灭活的详细描述。 Kv2.1 / Kv9.3异聚体从中间闭合状态以快速和完全的方式失活,但从打开状态以缓慢和不完全的方式失活。根据提出的定性模型,可以通过部分激活或去激活来接近通道门的中间关闭状态。这些过渡是Kv2.1 / Kv9.3失活的速率限制。最后,基于动力学的描述,我们提出了大鼠心脏中Kv2.1 / Kv9.3异构体的推定功能。

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