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果蝇中高盐味觉的分子机制。

A molecular mechanism for high salt taste in Drosophila.

机构信息

Department of Zoology and Life Sciences Institute, The University of British Columbia, Vancouver, BC V6T 1Z3, Canada.

Department of Zoology and Life Sciences Institute, The University of British Columbia, Vancouver, BC V6T 1Z3, Canada.

出版信息

Curr Biol. 2022 Jul 25;32(14):3070-3081.e5. doi: 10.1016/j.cub.2022.06.012. Epub 2022 Jun 29.

DOI:10.1016/j.cub.2022.06.012
PMID:35772408
Abstract

Dietary salt detection and consumption are crucial to maintaining fluid and ionic homeostasis. To optimize salt intake, animals employ salt-dependent activation of multiple taste pathways. Generally, sodium activates attractive taste cells, but attraction is overridden at high salt concentrations by cation non-selective activation of aversive taste cells. In flies, high salt avoidance is driven by both "bitter" taste neurons and a class of glutamatergic "high salt" neurons expressing pickpocket23 (ppk23). Although the cellular basis of salt taste has been described, many of the molecular mechanisms remain elusive. Here, we show that ionotropic receptor 7c (IR7c) is expressed in glutamatergic high salt neurons, where it functions with co-receptors IR76b and IR25a to detect high salt and is essential for monovalent salt taste. Misexpression of IR7c in sweet neurons, which endogenously express IR76b and IR25a, confers responsiveness to non-sodium salts, indicating that IR7c is sufficient to convert a sodium-selective gustatory receptor neuron to a cation non-selective one. Furthermore, the resultant transformation of taste neuron tuning switches potassium chloride from an aversive to an attractive tastant. This research provides insight into the molecular basis of monovalent and divalent salt-taste coding.

摘要

饮食盐的检测和摄入对于维持液体和离子内环境平衡至关重要。为了优化盐的摄入,动物采用盐依赖性激活多种味觉通路的方式。通常情况下,钠离子激活有吸引力的味觉细胞,但在高盐浓度下,阳离子非选择性激活厌恶味觉细胞会使吸引力减弱。在果蝇中,高盐回避既由“苦味”味觉神经元驱动,也由表达 pickpocket23 (ppk23)的一类谷氨酸能“高盐”神经元驱动。尽管盐味觉的细胞基础已经描述,但许多分子机制仍不清楚。在这里,我们表明离子型受体 7c (IR7c) 在谷氨酸能高盐神经元中表达,在这些神经元中,它与共受体 IR76b 和 IR25a 一起作用来检测高盐,并对单价盐味觉至关重要。IR7c 在甜神经元中的异位表达,这些神经元内源性表达 IR76b 和 IR25a,赋予了对非钠盐的反应性,表明 IR7c 足以将钠离子选择性味觉受体神经元转化为阳离子非选择性神经元。此外,味觉神经元调谐的这种转变将氯化钾从厌恶性味觉转变为有吸引力的味觉。这项研究为单价和二价盐味觉编码的分子基础提供了新的见解。

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