Department of Cell Biology, Dorris Neuroscience Center, The Scripps Research Institute, La Jolla, California 92037, USA.
Nature. 2012 Feb 19;483(7388):209-12. doi: 10.1038/nature10801.
Transduction of mechanical stimuli by receptor cells is essential for senses such as hearing, touch and pain. Ion channels have a role in neuronal mechanotransduction in invertebrates; however, functional conservation of these ion channels in mammalian mechanotransduction is not observed. For example, no mechanoreceptor potential C (NOMPC), a member of transient receptor potential (TRP) ion channel family, acts as a mechanotransducer in Drosophila melanogaster and Caenorhabditis elegans; however, it has no orthologues in mammals. Degenerin/epithelial sodium channel (DEG/ENaC) family members are mechanotransducers in C. elegans and potentially in D. melanogaster; however, a direct role of its mammalian homologues in sensing mechanical force has not been shown. Recently, Piezo1 (also known as Fam38a) and Piezo2 (also known as Fam38b) were identified as components of mechanically activated channels in mammals. The Piezo family are evolutionarily conserved transmembrane proteins. It is unknown whether they function in mechanical sensing in vivo and, if they do, which mechanosensory modalities they mediate. Here we study the physiological role of the single Piezo member in D. melanogaster (Dmpiezo; also known as CG8486). Dmpiezo expression in human cells induces mechanically activated currents, similar to its mammalian counterparts. Behavioural responses to noxious mechanical stimuli were severely reduced in Dmpiezo knockout larvae, whereas responses to another noxious stimulus or touch were not affected. Knocking down Dmpiezo in sensory neurons that mediate nociception and express the DEG/ENaC ion channel pickpocket (ppk) was sufficient to impair responses to noxious mechanical stimuli. Furthermore, expression of Dmpiezo in these same neurons rescued the phenotype of the constitutive Dmpiezo knockout larvae. Accordingly, electrophysiological recordings from ppk-positive neurons revealed a Dmpiezo-dependent, mechanically activated current. Finally, we found that Dmpiezo and ppk function in parallel pathways in ppk-positive cells, and that mechanical nociception is abolished in the absence of both channels. These data demonstrate the physiological relevance of the Piezo family in mechanotransduction in vivo, supporting a role of Piezo proteins in mechanosensory nociception.
感觉细胞对机械刺激的转导对于听觉、触觉和疼痛等感觉至关重要。离子通道在无脊椎动物的神经元机械转导中起作用;然而,这些离子通道在哺乳动物机械转导中的功能保守性尚未被观察到。例如,机械感受器电位 C(NOMPC),瞬时受体电位(TRP)离子通道家族的一员,在黑腹果蝇和秀丽隐杆线虫中充当机械感受器;然而,在哺乳动物中没有它的同源物。退行/上皮钠通道(DEG/ENaC)家族成员是秀丽隐杆线虫和潜在的黑腹果蝇中的机械感受器;然而,其哺乳动物同源物在感受机械力方面的直接作用尚未得到证明。最近,Piezo1(也称为 Fam38a)和 Piezo2(也称为 Fam38b)被鉴定为哺乳动物中机械激活通道的组成部分。Piezo 家族是进化上保守的跨膜蛋白。目前尚不清楚它们是否在体内的机械感应中发挥作用,如果是这样,它们介导哪种机械感觉模式。在这里,我们研究了果蝇(Dmpiezo;也称为 CG8486)中单个 Piezo 成员的生理作用。在人类细胞中表达 Dmpiezo 会诱导类似于其哺乳动物对应物的机械激活电流。在 Dmpiezo 敲除幼虫中,对有害机械刺激的行为反应严重降低,而对另一种有害刺激或触摸的反应不受影响。在介导伤害感受并表达 DEG/ENaC 离子通道 pickpocket(ppk)的感觉神经元中敲低 Dmpiezo 足以损害对有害机械刺激的反应。此外,在这些相同的神经元中表达 Dmpiezo 足以挽救组成型 Dmpiezo 敲除幼虫的表型。因此,从 ppk 阳性神经元进行的电生理记录显示出依赖于 Dmpiezo 的机械激活电流。最后,我们发现 Dmpiezo 和 ppk 在 ppk 阳性细胞中平行途径中起作用,并且在没有这两种通道的情况下,机械伤害感受被消除。这些数据表明 Piezo 家族在体内机械转导中的生理相关性,支持 Piezo 蛋白在机械感觉伤害感受中的作用。
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