Abstract
Like other autoimmune diseases, rheumatoid arthritis (RA) develops in distinct stages, with each phase of disease linked to immune cell dysfunction. HLA class II genes confer the strongest genetic risk to develop RA. They encode for molecules essential in the activation and differentiation of T cells, placing T cells upstream in the immunopathology. In Phase 1 of the RA disease process, T cells lose a fundamental function, their ability to be self-tolerant, and provide help for autoantibody-producing B cells. Phase 2 begins many years later, when mis-differentiated T cells gain tissue-invasive effector functions, enter the joint, promote non-resolving inflammation, and give rise to clinically relevant arthritis. In Phase 3 of the RA disease process, abnormal innate immune functions are added to adaptive autoimmunity, converting synovial inflammation into a tissue-destructive process that erodes cartilage and bone. Emerging data have implicated metabolic mis-regulation as a fundamental pathogenic pathway in all phases of RA. Early in their life cycle, RA T cells fail to repair mitochondrial DNA, resulting in a malfunctioning metabolic machinery. Mitochondrial insufficiency is aggravated by the mis-trafficking of the energy sensor AMPK away from the lysosomal surface. The metabolic signature of RA T cells is characterized by the shunting of glucose toward the pentose phosphate pathway and toward biosynthetic activity. During the intermediate and terminal phase of RA-imposed tissue inflammation, tissue-residing macrophages, T cells, B cells and stromal cells are chronically activated and under high metabolic stress, creating a microenvironment poor in oxygen and glucose, but rich in metabolic intermediates, such as lactate. By sensing tissue lactate, synovial T cells lose their mobility and are trapped in the tissue niche. The linkage of defective DNA repair, misbalanced metabolic pathways, autoimmunity, and tissue inflammation in RA encourages metabolic interference as a novel treatment strategy during both the early stages of tolerance breakdown and the late stages of tissue inflammation. Defining and targeting metabolic abnormalities provides a new paradigm to treat, or even prevent, the cellular defects underlying autoimmune disease.
Highlights
Rheumatoid arthritis (RA) is a chronic, systemic autoimmune disease characterized by inflammation of the synovial tissue and autoantibody production [1, 2]
The genetic risk conferred by HLA class II molecules, the accumulation of chronically activated T cells in the diseased joint and the T-cell dependence of autoantibody production all support a critical role of dysfunctional memory T cells as a salient feature of rheumatoid arthritis (RA)
One consequence of hypoxia is the activation of the transcription factor Hypoxia-inducible factor 1a (HIF-1a), which in turn promotes a gene program designed to enhance the production of glycolytic energy, including glucose transporters and glycolytic enzymes [76, 77]
Summary
Rheumatoid arthritis (RA) is a chronic, systemic autoimmune disease characterized by inflammation of the synovial tissue and autoantibody production [1, 2]. Differentiation and functional commitment of T cells is critically dependent on metabolic adaptations that co-ordinate the biosynthetic and energy demands imposed by chronic activation and the massive generation of cellular offspring [11]. These data support the concept that irregularities in glucose metabolism are evident during an early stage of RA, when naïve CD4+ T cells deviate from a normal differentiation pattern and make a commitment to become a pro-inflammatory effector cell.
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