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在细胞内钙离子成像实验中,弱刺激和强刺激引起的 TRP 通道介导反应的幅度之间缺乏相关性。

Lack of correlation between the amplitudes of TRP channel-mediated responses to weak and strong stimuli in intracellular Ca(2+) imaging experiments.

机构信息

Laboratory for Ion Channel Research and TRP Research Platform Leuven (TRPLe), Department of Molecular Cell Biology, KU Leuven, Belgium.

出版信息

Cell Calcium. 2013 Nov;54(5):362-74. doi: 10.1016/j.ceca.2013.08.005. Epub 2013 Sep 8.

Abstract

It is often observed in intracellular Ca(2+) imaging experiments that the amplitudes of the Ca(2+) signals elicited by newly characterized TRP agonists do not correlate with the amplitudes of the responses evoked subsequently by a specific potent agonist. We investigated this rather controversial phenomenon by first testing whether it is inherent to the comparison of the effects of weak and strong stimuli. Using five well-characterized TRP channel agonists in commonly used heterologous expression systems we found that the correlation between the amplitudes of the Ca(2+) signals triggered by two sequentially applied stimuli is only high when both stimuli are strong. Using mathematical simulations of intracellular Ca(2+) dynamics we illustrate that the innate heterogeneity in expression and functional properties of Ca(2+) extrusion (e.g. plasma membrane Ca(2+) ATPase) and influx (TRP channels) pathways across a cellular population is a sufficient condition for low correlation between the amplitude of Ca(2+) signals elicited by weak and strong stimuli. Taken together, our data demonstrate that this phenomenon is an expected outcome of intracellular Ca(2+) imaging experiments that cannot be taken as evidence for lack of specificity of low-efficacy stimuli, or as an indicator of the need of other cellular components for channel stimulation.

摘要

在细胞内 Ca(2+) 成像实验中,经常观察到新表征的 TRP 激动剂引起的 Ca(2+)信号幅度与随后由特定有效激动剂引起的反应幅度不相关。我们通过首先测试这种相当有争议的现象是否固有于弱刺激和强刺激的比较来研究这个问题。我们使用五个在常用异源表达系统中充分表征的 TRP 通道激动剂发现,当两个刺激都很强时,两个顺序施加的刺激引发的 Ca(2+)信号幅度之间的相关性才很高。我们通过细胞内 Ca(2+)动力学的数学模拟说明了 Ca(2+)外排(例如质膜 Ca(2+)ATP 酶)和流入(TRP 通道)途径在细胞群体中的表达和功能特性固有异质性是弱刺激和强刺激引发的 Ca(2+)信号幅度之间低相关性的充分条件。总之,我们的数据表明,这种现象是细胞内 Ca(2+)成像实验的预期结果,不能将其作为低效能刺激缺乏特异性的证据,也不能作为通道刺激需要其他细胞成分的指标。

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