4.5 Review

Cardiovascular effects of approved drugs for rheumatoid arthritis

Journal

NATURE REVIEWS RHEUMATOLOGY
Volume 17, Issue 5, Pages 270-290

Publisher

NATURE PORTFOLIO
DOI: 10.1038/s41584-021-00593-3

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Various drugs used in the management of rheumatoid arthritis have anti-inflammatory effects that can hinder atherosclerosis development, but they may also increase cardiovascular risk. While controlling inflammation can reduce the progression of atherosclerosis, some drugs may also directly or indirectly promote atherosclerosis. The primary objective for clinicians should be disease control, selecting the most appropriate drug for each patient while considering joint and cardiovascular outcomes.
Various drugs used in rheumatoid arthritis management have anti-inflammatory effects that can hinder atherosclerosis development and progression. However, these drugs can also concurrently have different pro-atherogenic effects, complicating the relationship between these drugs and cardiovascular involvement in rheumatoid arthritis. The risk of cardiovascular disease is increased in patients with rheumatoid arthritis compared with the general population owing to the influence of traditional and non-traditional risk factors. Inflammation has a pivotal contribution and can accelerate the atherosclerotic process. Although dampening inflammation with DMARDs should theoretically abrogate this process, evidence suggests that these drugs can also promote atherosclerosis directly and indirectly, hence adding to an increased cardiovascular burden. However, the extent and direction of the effects largely differ across drugs. Understanding how these drugs influence endothelial damage and vascular repair mechanisms is key to understanding these outcomes. NSAIDs and glucocorticoids can increase the cardiovascular risk. Conversely, conventional, biologic and targeted DMARDs control inflammation and reduce this risk, although some of these drugs can also aggravate traditional factors or thrombotic events. Given these data, the fundamental objective for clinicians should be disease control, in an individualized approach that considers the most appropriate drug for each patient, taking into account joint and cardiovascular outcomes. This Review provides a comprehensive analysis of the effects of DMARDs and other approved drugs on cardiovascular involvement in rheumatoid arthritis, from a clinical and mechanistic perspective, with a roadmap to inform the research agenda.

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