- Gyoneva, Stefka;
- Hosur, Raghavendra;
- Gosselin, David;
- Zhang, Baohong;
- Ouyang, Zhengyu;
- Cotleur, Anne C;
- Peterson, Michael;
- Allaire, Norm;
- Challa, Ravi;
- Cullen, Patrick;
- Roberts, Chris;
- Miao, Kelly;
- Reynolds, Taylor L;
- Glass, Christopher K;
- Burkly, Linda;
- Ransohoff, Richard M
CX3CR1, one of the highest expressed genes in microglia in mice and humans, is implicated in numerous microglial functions. However, the molecular mechanisms underlying Cx3cr1 signaling are not well understood. Here, we analyzed transcriptomes of Cx3cr1-deficient microglia under varying conditions by RNA-sequencing (RNA-seq). In 2-mo-old mice, Cx3cr1 deletion resulted in the down-regulation of a subset of immune-related genes, without substantial epigenetic changes in markers of active chromatin. Surprisingly, Cx3cr1-deficient microglia from young mice exhibited a transcriptome consistent with that of aged Cx3cr1-sufficient animals, suggesting a premature aging transcriptomic signature. Immunohistochemical analysis of microglia in young and aged mice revealed that loss of Cx3cr1 modulates microglial morphology in a comparable fashion. Our results suggest that CX3CR1 may regulate microglial function in part by modulating the expression levels of a subset of inflammatory genes during chronological aging, making Cx3cr1-deficient mice useful for studying aged microglia.