首页> 外文期刊>Neuroscience Letters: An International Multidisciplinary Journal Devoted to the Rapid Publication of Basic Research in the Brain Sciences >Genetic recombination in disgust-associated bitter taste-responsive neurons of the central nucleus of amygdala in male mice
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Genetic recombination in disgust-associated bitter taste-responsive neurons of the central nucleus of amygdala in male mice

机译:雄性小鼠中央核的厌恶相关苦味响应神经元的遗传重组

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摘要

A bitter substance induces specific orofacial and somatic behavioral reactions such as gapes in mice as well as monkeys and humans. These reactions have been proposed to represent affective disgust, and therefore, understanding the neuronal basis of the reactions would pave the way to understand affective disgust. It is crucial to identify and access the specific neuronal ensembles that are activated by bitter substances, such as quinine, the intake of which induces disgust reactions. However, the method to access the quinine-activated neurons has not been fully established yet. Here, we show evidence that a targeted recombination in active populations (TRAP) method, induces genetic recombination in the quinine-activated neurons in the central nucleus of the amygdala (CeA). CeA is one of the well-known emotional centers of the brain. We found that the intraoral quinine infusion, that resulted in disgust reactions, increased both cFos-positive cells and Arc-positive cells in the CeA. By using Arc-CreER;Ai3 TRAP mice, we induced genetic recombination in the quinine-activated neurons and labelled them with fluorescent protein. We confirmed that the quinine-TRAPed fluorescently-labelled cells preferentially coexpressed Arc after quinine infusion. Our results suggest that the TRAP method can be used to access specific functional neurons in the CeA.
机译:苦味物质会诱发特定的口腔面部和躯体行为反应,如小鼠、猴子和人类的口吃。这些反应被认为代表情感厌恶,因此,理解这些反应的神经元基础将为理解情感厌恶铺平道路。识别和获取由苦味物质(如奎宁)激活的特定神经元群至关重要,奎宁的摄入会引起厌恶反应。然而,获取奎宁激活神经元的方法尚未完全建立。在这里,我们展示的证据表明,在活动群体中的靶向重组(TRAP)方法,在杏仁体中央核(CeA)的奎宁激活神经元中诱导基因重组。CeA是众所周知的大脑情感中心之一。我们发现,口服奎宁导致恶心反应,增加了CeA中的cFos阳性细胞和Arc阳性细胞。采用弧形筛;Ai3陷阱小鼠,我们在奎宁激活的神经元中诱导基因重组,并用荧光蛋白标记它们。我们证实,注射奎宁后,奎宁标记的荧光标记细胞优先共表达Arc。我们的结果表明,TRAP方法可用于访问CeA中的特定功能神经元。

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