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小鼠烟碱型受体高分辨率单通道记录中的短暂开放。

Short openings in high resolution single channel recordings of mouse nicotinic receptors.

作者信息

Hallermann Stefan, Heckmann Sabine, Dudel Josef, Heckmann Manfred

机构信息

Physiologisches Institut, Hermann-Herder-Str. 7, D-79104 Freiburg i. Br., Germany.

出版信息

J Physiol. 2005 Mar 15;563(Pt 3):645-62. doi: 10.1113/jphysiol.2004.080606. Epub 2005 Jan 27.

Abstract

The temporal fine structure of single channel currents was studied to obtain information on how agonists open nicotinic acetylcholine receptor channels. Currents were recorded from mouse myoballs with quartz pipettes in the on-cell mode of the patch-clamp technique. With 62 kHz filter cut-off and root mean square (r.m.s.) noise levels as low as 1.45 pA at 200 mV hyperpolarization, events down to 6 micros duration could be resolved with negligible error rate. Three types of openings with mean durations of 750 micros, 89 micros and 4 micros were identified with 0.1-10 microM suberyldicholine (SubCh). The relative frequencies of the three types of openings were 84% for long, 5% for medium and 11% for short openings with 1 microM SubCh. Stability plots and single channel current amplitude comparisons suggest that the three types of openings arise from a homogenous channel population. Above 10 microM SubCh, the three types of openings could not be discerned because channel openings occurred too closely spaced and open channels were increasingly blocked. Three types of openings can be generated with a mechanistic receptor model with two unequal binding sites, short and medium openings arising from one or the other monoliganded state, and long openings from the fully liganded state of the receptor. Maximum likelihood fitting of the rate constants of this model directly to the sequence of observed open and shut times accurately predicted the main physiological properties of the receptors with 0.1 microM SubCh. However, fitting recordings with 0.1-10 microM SubCh simultaneously revealed that this model cannot reproduce the weak influence of SubCh concentration on the proportions of the three types of openings. Therefore we conclude that short and medium openings are unlikely to arise preferentially from one or the other monoliganded state of nicotinic acetylcholine receptor channels.

摘要

研究了单通道电流的时间精细结构,以获取有关激动剂如何打开烟碱型乙酰胆碱受体通道的信息。采用膜片钳技术的细胞贴附模式,用石英微管从小鼠肌球上记录电流。在200 mV超极化时,滤波器截止频率为62 kHz,均方根(r.m.s.)噪声水平低至1.45 pA,持续时间低至6微秒的事件能够以可忽略不计的错误率分辨出来。用0.1 - 10 μM的辛二酰胆碱(SubCh)可识别出三种平均持续时间分别为750微秒、89微秒和4微秒的开放类型。对于1 μM的SubCh,三种开放类型的相对频率分别为长开放84%、中开放5%和短开放11%。稳定性图和单通道电流幅度比较表明,这三种开放类型源自同质的通道群体。高于10 μM的SubCh时,无法分辨出这三种开放类型,因为通道开放间隔太近,且开放通道越来越多地被阻断。具有两个不等结合位点的机制性受体模型可以产生三种开放类型,短开放和中开放分别源于一个或另一个单配体状态,长开放源于受体的完全配体状态。将该模型的速率常数直接对观察到的开放和关闭时间序列进行最大似然拟合,准确预测了0.1 μM SubCh时受体的主要生理特性。然而,同时对0.1 - 10 μM SubCh的记录进行拟合发现,该模型无法重现SubCh浓度对三种开放类型比例的微弱影响。因此我们得出结论,烟碱型乙酰胆碱受体通道的短开放和中开放不太可能优先源于一个或另一个单配体状态。

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