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Multi-Scale Molecular Deconstruction of the Serotonin Neuron System

机译:血清素神经元系统的多尺度分子解构

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Serotonergic (5HT) neurons modulate diverse behaviors and physiology and are implicated in distinct clinical disorders. Corresponding diversity in 5HT neuronal phenotypes is becoming apparent and is likely rooted in molecular differences, yet a comprehensive approach characterizing molecular variation across the 5HT system is lacking, as is concomitant linkage to cellular phenotypes. Here we combine intersectional fate mapping, neuron sorting, and genome-wide RNA-seq to deconstruct the mouse 5HT system at multiple levels of granularity-from anatomy, to genetic sublineages, to single neurons. Our unbiased analyses reveal principles underlying system organization, 5HT neuron subtypes, constellations of differentially expressed genes distinguishing subtypes, and predictions of subtype-specific functions. Using electrophysiology, subtype-specific neuron silencing, and conditional gene knockout, we show that these molecularly defined 5HT neuron subtypes are functionally distinct. Collectively, this resource classifies molecular diversity across the 5HT system and discovers sertonergic subtypes, markers, organizing principles, and subtype-specific functions with potential disease relevance.
机译:血清神经营养素(5HT)神经元调节各种行为和生理,并参与不同的临床疾病。 5HT神经元表型的相应多样性正在变得明显,并且很可能源于分子差异,但缺乏表征整个5HT系统分子变异的全面方法,也缺乏与细胞表型的伴随联系。在这里,我们结合了交叉命运映射,神经元分类和全基因组RNA-seq,以从粒度,解剖结构,遗传亚谱系到单个神经元的多个粒度解构鼠标5HT系统。我们的无偏见分析揭示了系统组成的基本原理,5HT神经元亚型,区分亚型的差异表达基因的星座以及对亚型特定功能的预测。使用电生理,亚型特异性神经元沉默和条件基因敲除,我们表明这些分子定义的5HT神经元亚型在功能上是不同的。总体而言,该资源对5HT系统中的分子多样性进行了分类,并发现了与潜在疾病相关的血清素能亚型,标志物,组织原理和亚型特异性功能。

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