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Pore dilation occurs in TRPA1 but not in TRPM8 channels

机译:孔扩张发生在TRPA1中,但不在TRPM8通道中发生

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摘要

Abundantly expressed in pain-sensing neurons, TRPV1, TRPA1 and TRPM8 are major cellular sensors of thermal, chemical and mechanical stimuli. The function of these ion channels has been attributed to their selective permeation of small cations (e.g., Ca2+, Na+ and K+), and the ion selectivity has been assumed to be an invariant fingerprint to a given channel. However, for TRPV1, the notion of invariant ion selectivity has been revised recently. When activated, TRPV1 undergoes time and agonist-dependent pore dilation, allowing permeation of large organic cations such as Yo-Pro and NMDG+. The pore dilation is of physiological importance, and has been exploited to specifically silence TRPV1-positive sensory neurons. It is unknown whether TRPA1 and TRPM8 undergo pore dilation. Here we show that TRPA1 activation by reactive or non-reactive agonists induces Yo-Pro uptake, which can be blocked by TRPA1 antagonists. In outside-out patch recordings using NMDG+ as the sole external cation and Na+ as the internal cation, TRPA1 activation results in dynamic changes in permeability to NMDG+. In contrast, TRPM8 activation does not produce either Yo-Pro uptake or significant change in ion selectivity. Hence, pore dilation occurs in TRPA1, but not in TRPM8 channels.
机译:TRPV1,TRPA1和TRPM8在痛觉神经元中大量表达,是热,化学和机械刺激的主要细胞传感器。这些离子通道的功能归因于它们对小阳离子(例如Ca2 +,Na +和K +)的选择性渗透,并且已将离子选择性假定为给定通道的不变指纹。但是,对于TRPV1,不变离子选择性的概念最近得到了修订。激活后,TRPV1会经历时间和激动剂依赖性的孔扩张,从而允许大型有机阳离子(例如Yo-Pro和NMDG +)渗透。毛孔扩张具有重要的生理意义,并已被用来特异性沉默TRPV1阳性感觉神经元。尚不清楚TRPA1和TRPM8是否经历孔扩张。在这里,我们显示反应性或非反应性激动剂激活TRPA1会诱导Yo-Pro摄取,而TRPA1拮抗剂可以阻止Yo-Pro摄取。在使用NMDG +作为唯一的外部阳离子和Na +作为内部阳离子的外向面补丁记录中,TRPA1激活导致对NMDG +的渗透性动态变化。相反,TRPM8激活既不会产生Yo-Pro吸收,也不会产生离子选择性的显着变化。因此,孔扩张发生在TRPA1中,而不发生在TRPM8通道中。

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