1. K-RAS GTPase- and B-RAF kinase–mediated T-cell tolerance defects in rheumatoid arthritis
- Author
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Mingcan Yu, Guangjin Li, Karnail Singh, Sergey Pryshchep, Mary M. Cavanagh, Pratima Deshpande, Cornelia M. Weyand, and Jörg J. Goronzy
- Subjects
Proto-Oncogene Proteins B-raf ,MAPK/ERK pathway ,Cell signaling ,T-Lymphocytes ,T cell ,Arthritis ,Biology ,medicine.disease_cause ,GTP Phosphohydrolases ,Flow cytometry ,Immune tolerance ,Arthritis, Rheumatoid ,T-Lymphocyte Subsets ,Gene expression ,Immune Tolerance ,medicine ,Humans ,Extracellular Signal-Regulated MAP Kinases ,Multidisciplinary ,medicine.diagnostic_test ,medicine.disease ,Molecular biology ,Enzyme Activation ,Genes, ras ,medicine.anatomical_structure ,PNAS Plus ,KRAS - Abstract
Autoantibodies to common autoantigens and neoantigens, such as IgG Fc and citrullinated peptides, are immunological hallmarks of rheumatoid arthritis (RA). We examined whether a failure in maintaining tolerance is mediated by defects in T-cell receptor activation threshold settings. RA T cells responded to stimulation with significantly higher ERK phosphorylation ( P < 0.001). Gene expression arrays of ERK pathway members suggested a higher expression of KRAS and BRAF , which was confirmed by quantitative PCR ( P = 0.003), Western blot, and flow cytometry ( P < 0.01). Partial silencing of KRAS and BRAF lowered activation-induced phosphorylated ERK levels ( P < 0.01). In individual cells, levels of these signaling molecules correlated with ERK phosphorylation, attesting that their concentrations are functionally important. In confocal studies, B-RAF/K-RAS clustering was increased in RA T cells 2 min after T-cell receptor stimulation ( P < 0.001). Overexpression of B-RAF and K-RAS in normal CD4 T cells amplified polyclonal T-cell proliferation and facilitated responses to citrullinated peptides. We propose that increased expression of B-RAF and K-RAS lowers T-cell activation thresholds in RA T cells, enabling responses to autoantigens.
- Published
- 2012
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