Inhibition of Glycolysis in Pathogenic TH17 Cells through Targeting a miR -21-Peli1-c-Rel Pathway Prevents Autoimmunity.
Rong QiuXiang YuLi WangZhijun HanChao YaoYange CuiGuojun HouDai DaiWenfei JinNan ShenPublished in: Journal of immunology (Baltimore, Md. : 1950) (2020)
It is well known that some pathogenic cells have enhanced glycolysis; the regulatory network leading to increased glycolysis are not well characterized. In this study, we show that CNS-infiltrated pathogenic TH17 cells from diseased mice specifically upregulate glycolytic pathway genes compared with homeostatic intestinal TH17 cells. Bioenergetic assay and metabolomics analyses indicate that in vitro-derived pathogenic TH17 cells are highly glycolytic compared with nonpathogenic TH17 cells. Chromatin landscape analyses demonstrate TH17 cells in vivo that show distinct chromatin states, and pathogenic TH17 cells show enhanced chromatin accessibility at glycolytic genes with NF-κB binding sites. Mechanistic studies reveal that miR-21 targets the E3 ubiquitin ligase Peli1-c-Rel pathway to promote glucose metabolism of pathogenic TH17 cells. Therapeutic targeting c-Rel-mediated glycolysis in pathogenic TH17 cells represses autoimmune diseases. These findings extend our understanding of the regulation TH17 cell glycolysis in vivo and provide insights for future therapeutic intervention to TH17 cell-mediated autoimmune diseases.
Keyphrases
- induced apoptosis
- cell cycle arrest
- randomized controlled trial
- oxidative stress
- endoplasmic reticulum stress
- genome wide
- gene expression
- cell proliferation
- single cell
- cell death
- type diabetes
- long non coding rna
- blood brain barrier
- immune response
- dna methylation
- insulin resistance
- cancer therapy
- inflammatory response