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Defining Midbrain Dopaminergic Neuron Diversity by Single-Cell Gene Expression Profiling

机译:通过单细胞基因表达分析定义中脑多巴胺能神经元多样性

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摘要

Effective approaches to neuropsychiatric disorders require detailed understanding of the cellular composition and circuitry of the complex mammalian brain. Here, we present a paradigm for deconstructing the diversity of neurons defined by a specific neurotransmitter using a microfluidic dynamic array to simultaneously evaluate the expression of 96 genes in single neurons. With this approach, we successfully identified multiple molecularly distinct dopamine neuron subtypes and localized them in the adult mouse brain. To validate the anatomical and functional correlates of molecular diversity, we provide evidence that one Vip+ subtype, located in the periaqueductal region, has a discrete projection field within the extended amygdala. Another Aldh1a1+ subtype, located in the substantia nigra, is especially vulnerable in the 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP) model of Parkinson's disease. Overall, this rapid, cost-effective approach enables the identification and classification of multiple dopamine neuron subtypes, with distinct molecular, anatomical, and functional properties.
机译:神经精神疾病的有效方法需要详细了解复杂哺乳动物脑的细胞组合物和电路。在这里,我们提出了一种用于解构由微流体动态阵列的特异性神经递质由特定神经递质定义的神经元的多样性的范例同时评估单个神经元中的96基因的表达。通过这种方法,我们成功地鉴定了多种分子不同的多巴胺神经元亚型,并将其局限于成年小鼠脑中。为了验证分子多样性的解剖学和功能相关性,我们提供了一种证据表明,一个VIP +亚型,位于Periaquencental地区,在扩展的Amygdala内具有一个离散的投影场。位于位于Indicaia Nigra的另一个Aldh1a1 +亚型,特别容易受到帕金森病的1-甲基-4-苯基-1,2,3,6-四氢吡啶(MPTP)模型。总的来说,这种快速,经济有效的方法能够鉴定和分类多巴胺神经元亚型,具有不同的分子,解剖学和功能性。

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