| Literature DB >> 31710287 |
Stephen J Smith1, Uygar Sümbül1, Lucas T Graybuck1, Forrest Collman1, Sharmishtaa Seshamani1, Rohan Gala1, Olga Gliko1, Leila Elabbady1, Jeremy A Miller1, Trygve E Bakken1, Jean Rossier2, Zizhen Yao1, Ed Lein1, Hongkui Zeng1, Bosiljka Tasic1, Michael Hawrylycz1.
Abstract
Seeking new insights into the homeostasis, modulation and plasticity of cortical synaptic networks, we have analyzed results from a single-cell RNA-seq study of 22,439 mouse neocortical neurons. Our analysis exposes transcriptomic evidence for dozens of molecularly distinct neuropeptidergic modulatory networks that directly interconnect all cortical neurons. This evidence begins with a discovery that transcripts of one or more neuropeptide precursor (NPP) and one or more neuropeptide-selective G-protein-coupled receptor (NP-GPCR) genes are highly abundant in all, or very nearly all, cortical neurons. Individual neurons express diverse subsets of NP signaling genes from palettes encoding 18 NPPs and 29 NP-GPCRs. These 47 genes comprise 37 cognate NPP/NP-GPCR pairs, implying the likelihood of local neuropeptide signaling. Here, we use neuron-type-specific patterns of NP gene expression to offer specific, testable predictions regarding 37 peptidergic neuromodulatory networks that may play prominent roles in cortical homeostasis and plasticity.Entities:
Keywords: mouse; neocortex; neuromodulation; neuron types; neuropeptides; neuroscience; synaptic networks; transcriptomics
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Year: 2019 PMID: 31710287 PMCID: PMC6881117 DOI: 10.7554/eLife.47889
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140