Division of Cell Signaling, Okazaki Institute for Integrative Bioscience (National Institute for Physiological Sciences), National Institute of Natural Sciences, Okazaki, Aichi, 444-8787, Japan.
J Biol Chem. 2012 Aug 31;287(36):30743-54. doi: 10.1074/jbc.M112.362194. Epub 2012 Jul 12.
Transient receptor potential ankyrin 1 (TRPA1) and TRP vanilloid 1 (V1) perceive noxious temperatures and chemical stimuli and are involved in pain sensation in mammals. Thus, these two channels provide a model for understanding how different genes with similar biological roles may influence the function of one another during the course of evolution. However, the temperature sensitivity of TRPA1 in ancestral vertebrates and its evolutionary path are unknown as its temperature sensitivities vary among different vertebrate species. To elucidate the functional evolution of TRPA1, TRPA1s of the western clawed (WC) frogs and green anole lizards were characterized. WC frog TRPA1 was activated by heat and noxious chemicals that activate mammalian TRPA1. These stimuli also activated native sensory neurons and elicited nocifensive behaviors in WC frogs. Similar to mammals, TRPA1 was functionally co-expressed with TRPV1, another heat- and chemical-sensitive nociceptive receptor, in native sensory neurons of the WC frog. Green anole TRPA1 was also activated by heat and noxious chemical stimulation. These results suggest that TRPA1 was likely a noxious heat and chemical receptor and co-expressed with TRPV1 in the nociceptive sensory neurons of ancestral vertebrates. Conservation of TRPV1 heat sensitivity throughout vertebrate evolution could have changed functional constraints on TRPA1 and influenced the functional evolution of TRPA1 regarding temperature sensitivity, whereas conserving its noxious chemical sensitivity. In addition, our results also demonstrated that two mammalian TRPA1 inhibitors elicited different effect on the TRPA1s of WC frogs and green anoles, which can be utilized to clarify the structural bases for inhibition of TRPA1.
瞬时受体电位锚蛋白 1(TRPA1)和 TRP 香草素 1(V1)感知有害温度和化学刺激,并参与哺乳动物的疼痛感觉。因此,这两个通道为理解具有相似生物学作用的不同基因如何在进化过程中相互影响提供了一个模型。然而,由于其在不同脊椎动物物种中的温度敏感性不同,因此祖先脊椎动物中 TRPA1 的温度敏感性及其进化途径尚不清楚。为了阐明 TRPA1 的功能进化,对西方爪蟾(WC)青蛙和绿安乐蜥的 TRPA1 进行了特征描述。WC 青蛙 TRPA1 被热和激活哺乳动物 TRPA1 的有害化学物质激活。这些刺激还激活了本地感觉神经元,并在 WC 青蛙中引起伤害性行为。与哺乳动物相似,TRPA1 与另一种热和化学敏感的伤害性受体 TRPV1 在 WC 青蛙的本地感觉神经元中功能上共同表达。绿安乐蜥 TRPA1 也被热和有害的化学刺激激活。这些结果表明,TRPA1 可能是一种有害的热和化学受体,并且在祖先脊椎动物的伤害性感觉神经元中与 TRPV1 共同表达。TRPV1 热敏感性在整个脊椎动物进化过程中的保守性可能改变了 TRPA1 的功能约束,并影响了 TRPA1 关于温度敏感性的功能进化,而保持了其有害化学敏感性。此外,我们的结果还表明,两种哺乳动物 TRPA1 抑制剂对 WC 青蛙和绿安乐蜥的 TRPA1 产生了不同的影响,这可以用来阐明 TRPA1 抑制的结构基础。