Gao Lizhi, Mi Xianqiang, Paajanen Vesa, Wang Kun, Fan Zheng
Department of Physiology, University of Tennessee Health Science Center, Memphis, TN 38163, USA.
Proc Natl Acad Sci U S A. 2005 Dec 6;102(49):17630-5. doi: 10.1073/pnas.0505158102. Epub 2005 Nov 21.
X-ray structures of the bacterial K+ channel KcsA have led to unparalleled progress in our understanding of ion channel structures. The KcsA channel has therefore been a prototypic model used to study the structural basis of ion channel function, including the gating mechanism. This channel was previously found to close at near-neutral intracellular pH (pH(i)) and to open at acidic pH(i). Here, we report the presence of a previously unknown channel inactivation process that occurs after the KcsA channel is activated. In our experiments, mammalian cells transfected with a codon-optimized synthetic gene encoding the KcsA protein expressed K+-selective channels that activated in response to a decrease in pH(i). Using patch-clamp and rapid solution exchange techniques, we observed that the KcsA channels inactivated within hundreds of milliseconds after channel activation. At all tested pHs, inactivation always accompanied activation, and it was profoundly accelerated in the same pH range at which activation increased steeply. Recovery from inactivation was observed, and its extent depended on the pH(i) and the amount of time that the channel was inactive. KcsA channel inactivation can be described by a kinetic model in which pH(i) controls inactivation through pH-dependent activation. This heretofore-undocumented inactivation process increases the complexity of KcsA channel function, but it also offers a potential model for studying the structural correspondence of ion channel inactivation.
细菌钾离子通道KcsA的X射线结构使我们对离子通道结构的理解取得了前所未有的进展。因此,KcsA通道一直是用于研究离子通道功能结构基础(包括门控机制)的原型模型。此前发现该通道在接近中性的细胞内pH值(pH(i))时关闭,在酸性pH(i)时打开。在此,我们报告了KcsA通道激活后出现的一种此前未知的通道失活过程。在我们的实验中,用编码KcsA蛋白的密码子优化合成基因转染的哺乳动物细胞表达了对pH(i)降低有反应而激活的钾离子选择性通道。使用膜片钳和快速溶液交换技术,我们观察到KcsA通道在激活后数百毫秒内失活。在所有测试的pH值下,失活总是伴随着激活,并且在激活急剧增加的相同pH范围内失活显著加速。观察到了从失活状态的恢复,其程度取决于pH(i)和通道失活的时间。KcsA通道失活可以用一个动力学模型来描述,其中pH(i)通过pH依赖性激活来控制失活。这种迄今为止未被记录的失活过程增加了KcsA通道功能的复杂性,但它也为研究离子通道失活的结构对应关系提供了一个潜在模型。