UCLA Neurocardiology Research Center of Excellence, Los Angeles, California, USA.
UCLA Cardiac Arrhythmia Center, Los Angeles, California, USA.
Glia. 2021 May;69(5):1281-1291. doi: 10.1002/glia.23965. Epub 2021 Jan 12.
Stellate ganglion neurons, important mediators of cardiopulmonary neurotransmission, are surrounded by satellite glial cells (SGCs), which are essential for the function, maintenance, and development of neurons. However, it remains unknown whether SGCs in adult sympathetic ganglia exhibit any functional diversity, and what role this plays in modulating neurotransmission. We performed single-cell RNA sequencing of mouse stellate ganglia (n = 8 animals), focusing on SGCs (n = 11,595 cells). SGCs were identified by high expression of glial-specific transcripts, S100b and Fabp7. Microglia and Schwann cells were identified by expression of C1qa/C1qb/C1qc and Ncmap/Drp2, respectively, and excluded from further analysis. Dimensionality reduction and clustering of SGCs revealed six distinct transcriptomic subtypes, one of which was characterized the expression of pro-inflammatory markers and excluded from further analyses. The transcriptomic profiles and corresponding biochemical pathways of the remaining subtypes were analyzed and compared with published astrocytic transcriptomes. This revealed gradual shifts of developmental and functional pathways across the subtypes, originating from an immature and pluripotent subpopulation into two mature populations of SGCs, characterized by upregulated functional pathways such as cholesterol metabolism. As SGCs aged, these functional pathways were downregulated while genes and pathways associated with cellular stress responses were upregulated. These findings were confirmed and furthered by an unbiased pseudo-time analysis, which revealed two distinct trajectories involving the five subtypes that were studied. These findings demonstrate that SGCs in mouse stellate ganglia exhibit transcriptomic heterogeneity along maturation or differentiation axes. These subpopulations and their unique biochemical properties suggest dynamic physiological adaptations that modulate neuronal function.
星状神经节神经元是心肺神经传递的重要介质,它们被卫星胶质细胞(SGCs)包围,这些细胞对于神经元的功能、维持和发育至关重要。然而,目前尚不清楚成年交感神经节中的 SGC 是否表现出任何功能多样性,以及这种多样性在调节神经传递中扮演什么角色。我们对小鼠星状神经节(n=8 只动物)进行了单细胞 RNA 测序,重点关注 SGC(n=11595 个细胞)。SGC 通过高表达胶质特异性转录本 S100b 和 Fabp7 来识别。小胶质细胞和施万细胞通过表达 C1qa/C1qb/C1qc 和 Ncmap/Drp2 来识别,并排除在进一步分析之外。SGC 的降维和聚类揭示了六个不同的转录组亚型,其中一个亚型的特征是表达促炎标志物,并排除在进一步分析之外。对其余亚型的转录组谱和相应的生化途径进行了分析,并与已发表的星形胶质细胞转录组进行了比较。这揭示了发育和功能途径在整个亚型中的逐渐转变,从一个不成熟和多能的亚群转变为两个成熟的 SGC 群体,其特征是上调了胆固醇代谢等功能途径。随着 SGC 的老化,这些功能途径下调,而与细胞应激反应相关的基因和途径上调。这些发现通过无偏的伪时间分析得到了证实和进一步深化,该分析揭示了涉及五个亚型的两个不同轨迹。这些发现表明,小鼠星状神经节中的 SGC 沿着成熟或分化轴表现出转录组异质性。这些亚群及其独特的生化特性表明了调节神经元功能的动态生理适应。
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