| Literature DB >> 32091396 |
Eric Engelbrecht1, Michel V Levesque1, Liqun He2,3, Michael Vanlandewijck2,3, Anja Nitzsche4, Hira Niazi4, Andrew Kuo1, Sasha A Singh5, Masanori Aikawa5, Kristina Holton6, Richard L Proia7, Mari Kono7, William T Pu8,9, Eric Camerer4, Christer Betsholtz2,3, Timothy Hla1.
Abstract
Despite the medical importance of G protein-coupled receptors (GPCRs), in vivo cellular heterogeneity of GPCR signaling and downstream transcriptional responses are not understood. We report the comprehensive characterization of transcriptomes (bulk and single-cell) and chromatin domains regulated by sphingosine 1-phosphate receptor-1 (S1PR1) in adult mouse aortic endothelial cells. First, S1PR1 regulates NFκB and nuclear glucocorticoid receptor pathways to suppress inflammation-related mRNAs. Second, S1PR1 signaling in the heterogenous endothelial cell (EC) subtypes occurs at spatially-distinct areas of the aorta. For example, a transcriptomically distinct arterial EC population at vascular branch points (aEC1) exhibits ligand-independent S1PR1/ß-arrestin coupling. In contrast, circulatory S1P-dependent S1PR1/ß-arrestin coupling was observed in non-branch point aEC2 cells that exhibit an inflammatory gene expression signature. Moreover, S1P/S1PR1 signaling regulates the expression of lymphangiogenic and inflammation-related transcripts in an adventitial lymphatic EC (LEC) population in a ligand-dependent manner. These insights add resolution to existing concepts of endothelial heterogeneity, GPCR signaling and S1P biology.Entities:
Keywords: Sphingosine 1-phosphate; arterial endothelium; chromatin; chromosomes; endothelial cells; gene expression; lymphatic endothelium; mouse; transcriptome
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Year: 2020 PMID: 32091396 PMCID: PMC7054001 DOI: 10.7554/eLife.52690
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140