| First Author | McGill MM | Year | 2021 |
| Journal | Front Immunol | Volume | 12 |
| Pages | 715311 | PubMed ID | 34707603 |
| Mgi Jnum | J:312717 | Mgi Id | MGI:6785590 |
| Doi | 10.3389/fimmu.2021.715311 | Citation | McGill MM, et al. (2021) p38 MAP Kinase Signaling in Microglia Plays a Sex-Specific Protective Role in CNS Autoimmunity and Regulates Microglial Transcriptional States. Front Immunol 12:715311 |
| abstractText | Multiple sclerosis (MS) is an autoimmune demyelinating disease of the central nervous system, representing the leading cause of non-traumatic neurologic disease in young adults. This disease is three times more common in women, yet more severe in men, but the mechanisms underlying these sex differences remain largely unknown. MS is initiated by autoreactive T helper cells, but CNS-resident and CNS-infiltrating myeloid cells are the key proximal effector cells regulating disease pathology. We have previously shown that genetic ablation of p38alpha MAP kinase broadly in the myeloid lineage is protective in the autoimmune model of MS, experimental autoimmune encephalomyelitis (EAE), but only in females, and not males. To precisely define the mechanisms responsible, we used multiple genetic approaches and bone marrow chimeras to ablate p38alpha in microglial cells, peripheral myeloid cells, or both. Deletion of p38alpha in both cell types recapitulated the previous sex difference, with reduced EAE severity in females. Unexpectedly, deletion of p38alpha in the periphery was protective in both sexes. In contrast, deletion of p38alpha in microglia exacerbated EAE in males only, revealing opposing roles of p38alpha in microglia vs. periphery. Bulk transcriptional profiling revealed that p38alpha regulated the expression of distinct gene modules in male vs. female microglia. Single-cell transcriptional analysis of WT and p38alpha-deficient microglia isolated from the inflamed CNS revealed a diversity of complex microglial states, connected by distinct convergent transcriptional trajectories. In males, microglial p38alpha deficiency resulted in enhanced transition from homeostatic to disease-associated microglial states, with the downregulation of regulatory genes such as Atf3, Rgs1, Socs3, and Btg2, and increased expression of inflammatory genes such as Cd74, Trem2, and MHC class I and II genes. In females, the effect of p38alpha deficiency was divergent, exhibiting a unique transcriptional profile that included an upregulation of tissue protective genes, and a small subset of inflammatory genes that were also upregulated in males. Taken together, these results reveal a p38alpha-dependent sex-specific molecular pathway in microglia that is protective in CNS autoimmunity in males, suggesting that autoimmunity in males and females is driven by distinct cellular and molecular pathways, thus suggesting design of future sex-specific therapeutic approaches. |
