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天然产生的防御性烯醛化合物激活TRPA1。

Naturally Produced Defensive Alkenal Compounds Activate TRPA1.

作者信息

Blair Nathaniel T, Philipson Benjamin I, Richards Paige M, Doerner Julia F, Segura Abraham, Silver Wayne L, Clapham David E

机构信息

Howard Hughes Medical Institute (HHMI), Boston, MA, USA, Department of Cardiology, Boston Children's Hospital, Boston, MA 02115, USA, Department of Neurobiology, Harvard Medical School, Boston, MA 02115, USA.

Harvard College, Cambridge, MA 02138, USA.

出版信息

Chem Senses. 2016 May;41(4):281-92. doi: 10.1093/chemse/bjv071. Epub 2016 Feb 3.

Abstract

(E)-2-alkenals are aldehydes containing an unsaturated bond between the alpha and beta carbons. 2-alkenals are produced by many organisms for defense against predators and secretions containing (E)-2-alkenals cause predators to stop attacking and allow the prey to escape. Chemical ecologists have described many alkenal compounds with 3-20 carbons common, having varied positions of double bonds and substitutions. How do these defensive alkenals act to deter predators? We have tested the effects of (E)-2-alkenals with 6-12 carbons on transient receptor potential channels (TRP) commonly found in sensory neurons. We find that (E)-2-alkenals activate transient receptor potential ankyrin subtype 1 (TRPA1) at low concentrations-EC50s 10-100 µM (in 0 added Ca(2+) external solutions). Other TRP channels were either weakly activated (TRPV1, TRPV3) or insensitive (TRPV2, TRPV4, TRPM8). (E)-2-alkenals may activate TRPA1 by modifying cysteine side chains. However, target cysteines include others beyond the 3 in the amino-terminus implicated in activation, as a channel with cysteines at 621, 641, 665 mutated to serine responded robustly. Related chemicals, including the aldehydes hexanal and decanal, and (E)-2-hexen-1-ol also activated TRPA1, but with weaker potency. Rat trigeminal nerve recordings and behavioral experiments showed (E)-2-hexenal was aversive. Our results suggest that TRPA1 is likely a major target of these commonly used defensive chemicals.

摘要

(E)-2-烯醛是一类在α和β碳原子之间含有不饱和键的醛类化合物。许多生物体都会产生2-烯醛用于抵御捕食者,含有(E)-2-烯醛的分泌物会使捕食者停止攻击并让猎物逃脱。化学生态学家已经描述了许多常见的含有3至20个碳原子的烯醛化合物,它们具有不同的双键位置和取代基。这些防御性烯醛是如何起到威慑捕食者的作用的呢?我们测试了含有6至12个碳原子的(E)-2-烯醛对感觉神经元中常见的瞬时受体电位通道(TRP)的影响。我们发现,(E)-2-烯醛在低浓度下(在无添加Ca(2+)的外部溶液中,EC50为10-100μM)可激活瞬时受体电位锚蛋白1型(TRPA1)。其他TRP通道要么被微弱激活(TRPV1、TRPV3),要么不敏感(TRPV2、TRPV4、TRPM8)。(E)-2-烯醛可能通过修饰半胱氨酸侧链来激活TRPA1。然而,目标半胱氨酸包括氨基末端中参与激活的3个以外的其他半胱氨酸,因为一个将621、641、665位的半胱氨酸突变为丝氨酸的通道仍能强烈响应。相关化学物质,包括己醛、癸醛以及(E)-2-己烯-1-醇也能激活TRPA1,但效力较弱。大鼠三叉神经记录和行为实验表明,(E)-2-己烯醛具有厌恶作用。我们的结果表明,TRPA1可能是这些常用防御性化学物质的主要靶点。

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