Abstract
Autoimmune diseases affect roughly 5-10% of the total population, with women affected more than men. The standard treatment for autoimmune or autoinflammatory diseases had long been immunosuppressive agents until the advent of immunomodulatory biologic drugs, which aimed at blocking inflammatory mediators, including proinflammatory cytokines. At the frontier of these biologic drugs are TNF-α blockers. These therapies inhibit the proinflammatory action of TNF-α in common autoimmune diseases such as rheumatoid arthritis, psoriasis, ulcerative colitis, and Crohn’s disease. TNF-α blockade quickly became the “standard of care” for these autoimmune diseases due to their effectiveness in controlling disease and decreasing patient’s adverse risk profiles compared to broad-spectrum immunosuppressive agents. However, anti-TNF-α therapies have limitations, including known adverse safety risk, loss of therapeutic efficacy due to drug resistance, and lack of efficacy in numerous autoimmune diseases, including multiple sclerosis. The next wave of truly transformative therapeutics should aspire to provide a cure by selectively suppressing pathogenic autoantigen-specific immune responses while leaving the rest of the immune system intact to control infectious diseases and malignancies. In this review, we will focus on three main areas of active research in immune tolerance. First, tolerogenic vaccines aiming at robust, lasting autoantigen-specific immune tolerance. Second, T cell therapies using Tregs (either polyclonal, antigen-specific, or genetically engineered to express chimeric antigen receptors) to establish active dominant immune tolerance or T cells (engineered to express chimeric antigen receptors) to delete pathogenic immune cells. Third, IL-2 therapies aiming at expanding immunosuppressive regulatory T cells in vivo.
Highlights
The mammalian immune system evolved to protect our bodies from foreign pathogens and intrinsic aberrant malignancies while concurrently preventing deleterious immune responses toward self [1]
Engineered versions of IL-2 to modify the activity and binding specificity to T Regulatory Cell (Treg) versus non-Tregs and IL-2 complexed with anti-IL-2 antibody that indirectly impacts activity and selectivity to the high affinity IL2 receptor are among these approaches
Due to the mutations that inhibit interaction between IL-2 and CD122/CD132, these IL-2 muteins induced weaker STAT5 activation compared to wildtype IL-2 (WT)
Summary
The mammalian immune system evolved to protect our bodies from foreign pathogens and intrinsic aberrant malignancies while concurrently preventing deleterious immune responses toward self [1]. A tolerogenic vaccine comprised of IFN-b + MOG35-55 in Alum ameliorated MOG35-55-induced EAE in C57BL/6 mice when administered at peak disease [125]. Other tolerogenic vaccine strategies included fusing myelin peptides to the immunosuppressive S-antigen from Plasmodium falciparum [128] or targeting myelin peptides with the viral adhesion protein ps1, to M cells, which mediate mucosal antigen sampling and mucosal tolerance, to suppress EAE (Table 2) [129, 130].
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