| Literature DB >> 33264626 |
Samantha M Golomb1, Ian H Guldner1, Anqi Zhao1, Qingfei Wang1, Bhavana Palakurthi1, Emilija A Aleksandrovic1, Jacqueline A Lopez2, Shaun W Lee3, Kai Yang4, Siyuan Zhang5.
Abstract
Phenotypic and functional plasticity of brain immune cells contribute to brain tissue homeostasis and disease. Immune cell plasticity is profoundly influenced by tissue microenvironment cues and systemic factors. Aging and gut microbiota dysbiosis that reshape brain immune cell plasticity and homeostasis has not been fully delineated. Using Cellular Indexing of Transcriptomes and Epitopes by sequencing (CITE-seq), we analyze compositional and transcriptional changes of the brain immune landscape in response to aging and gut dysbiosis. Discordance between canonical surface-marker-defined immune cell types and their transcriptomes suggest transcriptional plasticity among immune cells. Ly6C+ monocytes predominate a pro-inflammatory signature in the aged brain, while innate lymphoid cells (ILCs) shift toward an ILC2-like profile. Aging increases ILC-like cells expressing a T memory stemness (Tscm) signature, which is reduced through antibiotics-induced gut dysbiosis. Systemic changes due to aging and gut dysbiosis increase propensity for neuroinflammation, providing insights into gut dysbiosis in age-related neurological diseases.Entities:
Keywords: CITE-seq; CNS; aging; brain; brain immunity; dysbiosis; gut microbiota; single-cell sequencing
Mesh:
Year: 2020 PMID: 33264626 PMCID: PMC7737488 DOI: 10.1016/j.celrep.2020.108438
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423