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含Kv1.1的通道对于动作电位起始期间的时间精确性至关重要。

Kv1.1-containing channels are critical for temporal precision during spike initiation.

作者信息

Gittelman Joshua X, Tempel Bruce L

机构信息

Neurobiology and Behaviour Program, University of Washington, Seattle, WA 98195, USA.

出版信息

J Neurophysiol. 2006 Sep;96(3):1203-14. doi: 10.1152/jn.00092.2005. Epub 2006 May 3.

Abstract

Low threshold, voltage-gated potassium currents (Ikl) are widely expressed in auditory neurons that can fire temporally precise action potentials (APs). In the medial nucleus of the trapezoid body (MNTB), channels containing the Kv1.1 subunit (encoded by the Kcna1 gene) underlie Ikl. Using pharmacology, genetics and whole cell patch-clamp recordings in mouse brain slices, we tested the role of Ikl in limiting AP latency-variability (jitter) in response to trains of single inputs at moderate to high stimulation rates. With dendrotoxin-K (DTX-K, a selective blocker of Kv1.1-containing channels), we blocked Ikl maximally (approximately 80% with 100 nM DTX-K) or partially (approximately 50% with 1-h incubation in 3 nM DTX-K). Ikl was similar in 3 nM DTX-K-treated cells and cells from Kcna1(-/-) mice, allowing a comparison of these two different methods of Ikl reduction. In response to current injection, Ikl reduction increased the temporal window for AP initiation and increased jitter in response to the smallest currents that were able to drive APs. While 100 nM DTX-K caused the largest increases, latency and jitter in Kcna1(-/-) cells and in 3 nM DTX-K-treated cells were similar to each other but increased compared with +/+. The near-phenocopy of the Kcna1(-/-) cells with 3 nM DTX-K shows that acute blockade of a subset of the Kv1.1-containing channels is functionally similar to the chronic elimination of all Kv1.1 subunits. During rapid stimulation (100-500 Hz), Ikl reduction increased jitter in response to both large and small inputs. These data show that Ikl is critical for maintaining AP temporal precision at physiologically relevant firing rates.

摘要

低阈值电压门控钾电流(Ikl)广泛表达于能够产生时间精确动作电位(APs)的听觉神经元中。在梯形体内侧核(MNTB)中,含有Kv1.1亚基(由Kcna1基因编码)的通道构成了Ikl。我们运用药理学、遗传学方法以及对小鼠脑片进行全细胞膜片钳记录,测试了Ikl在中等至高刺激速率下对单个输入序列作出反应时限制AP潜伏期变异性(抖动)的作用。使用树突毒素-K(DTX-K,一种含Kv1.1通道的选择性阻滞剂),我们最大程度地阻断了Ikl(100 nM DTX-K时约为80%)或部分阻断(3 nM DTX-K中孵育1小时约为50%)。在3 nM DTX-K处理的细胞和Kcna1(-/-)小鼠的细胞中,Ikl相似,这使得我们能够比较这两种降低Ikl的不同方法。对电流注入的反应中,Ikl的降低增加了AP起始的时间窗口,并增加了对能够驱动AP的最小电流的反应中的抖动。虽然100 nM DTX-K引起的增加最大,但Kcna1(-/-)细胞和3 nM DTX-K处理的细胞中的潜伏期和抖动彼此相似,但与+/+细胞相比增加了。3 nM DTX-K处理的细胞与Kcna1(-/-)细胞近乎表型相似,表明对含Kv1.1通道的一个亚群的急性阻断在功能上类似于对所有Kv1.1亚基的慢性消除。在快速刺激(100 - 500 Hz)期间,Ikl的降低增加了对大小输入的反应中的抖动。这些数据表明,Ikl对于在生理相关的放电速率下维持AP的时间精确性至关重要。

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