Although the specific trigger of the autoimmune response in rheumatoid arthritis (RA) is not known, it is generally believed the pathogenesis of RA is associated with the induction of inflammation via interactions of innate and the adaptive immune system. The main inflammatory mediators of joint inflammation and destruction in RA are tumor necrosis factor (TNF)-alpha, interleukin-1 (IL-1), IL-6, chemokines, and proteases. Advances in our understanding of the key cells and inflammatory cytokines have led to the development of targeted biologic agents. Recently, TH17 cells were characterized as a novel CD4+subset that preferentially produces IL-17, and IL-22 as the signature cytokines. TH17 cells appear to play a critical role in sustaining the inflammatory response and their presence is closely associated with autoimmune disease, which makes them an attractive therapeutic target. At present, 5 TNF-alpha inhibitors are approved for use by the FDA: infliximab, etanercept, adalimumab, golimumab, and certolizumab pegol, and all of these agents have been shown to be effective in reducing clinical signs of inflammation in RA patients. Multiple studies have demonstrated significant benefits of early treatment with TNF-alpha inhibitors combined with methotrexate. Other FDA-approved biologic agents for treating moderate-to-severe RA include abatacept, rituximab, and tocilizumab. All biologic agents carry an increased risk of infections. Following a greater understanding of the pathogenesis of RA, the treatment of this chronic disease has improved with the availability of biological agents targeting key molecules.