Host-derived mannose glycans trigger a pathogenic γδ T cell/IL-17a axis in autoimmunity.
Inês AlvesBeatriz Santos-PereiraNoelia de la CruzAna CamparVanda PintoPedro M RodriguesMarco AraújoSofia SantosJavier Ramos-SorianoCarlos VasconcelosRoberto SilvaNuno AfonsoFilipe Santos MiraCristina C BarriasMartin R GoodierJavier RojoLélita SantosAntónio MarinhoSalomé Soares PinhoPublished in: Science translational medicine (2023)
Autoimmune diseases are life-threatening disorders that cause increasing disability over time. Systemic lupus erythematosus (SLE) and other autoimmune diseases arise when immune stimuli override mechanisms of self-tolerance. Accumulating evidence has demonstrated that protein glycosylation is substantially altered in autoimmune disease development, but the mechanisms by which glycans trigger these autoreactive immune responses are still largely unclear. In this study, we found that presence of microbial-associated mannose structures at the surface of the kidney triggers the recognition of DC-SIGN-expressing γδ T cells, inducing a pathogenic interleukin-17a (IL-17a)-mediated autoimmune response. Mice lacking Mgat5 , which have a higher abundance of mannose structures in the kidney, displayed increased γδ T cell infiltration into the kidney that was associated with spontaneous development of lupus in older mice. N -acetylglucosamine supplementation, which promoted biosynthesis of tolerogenic branched N-glycans in the kidney, was found to inhibit γδ T cell infiltration and control disease development. Together, this work reveals a mannose-γδ T cell-IL-17a axis in SLE immunopathogenesis and highlights glycometabolic reprogramming as a therapeutic strategy for autoimmune disease treatment.
Keyphrases
- systemic lupus erythematosus
- disease activity
- multiple sclerosis
- dendritic cells
- immune response
- high resolution
- high fat diet induced
- rheumatoid arthritis
- cell surface
- physical activity
- regulatory t cells
- type diabetes
- microbial community
- toll like receptor
- middle aged
- mass spectrometry
- wild type
- insulin resistance
- community dwelling
- binding protein
- antibiotic resistance genes
- anaerobic digestion