Some disease-modifying antirheumatic drugs that are taken for rheumatoid arthritis or psoriasis appear to reduce the rate of incident diabetes, according to a report in the June 22/29 issue of JAMA.
In a retrospective cohort study of patients who had RA or psoriasis, the use of a tumor necrosis factor (TNF) inhibitor or hydroxychloroquine to treat the systemic inflammatory disorder was associated with a reduced risk of developing diabetes, compared with the use of methotrexate or nonbiologic DMARDs, said Dr. Daniel H. Solomon of the divisions of pharmacoepidemiology and rheumatology at Brigham and Women’s Hospital, Boston, and his associates.
"Considering these results, in light of prior findings regarding improved insulin and glucose metabolism and reduced diabetes risk with hydroxychloroquine and TNF inhibitors, there is evidence suggesting a possible role for DMARDs and immunosuppression in diabetes prevention," they noted.
The investigators assessed the relationship between DMARDs and the risk of new-onset diabetes because previous studies have demonstrated that inflammatory conditions such as RA and psoriasis predispose patients to insulin resistance, and that some of these anti-inflammatory medications appear to improve insulin resistance and prevent the onset of diabetes. They analyzed information from the databases of a Canadian health care system and a commercial U.S. health plan to identify 13,905 adults with RA or psoriasis who had filled at least one prescription for a DMARD and could be followed for approximately 6 months.
The DMARDs were divided into four mutually exclusive groups: TNF inhibitors such as adalimumab, etanercept, or infliximab; methotrexate; hydroxychloroquine; and other nonbiologic DMARDs such as sulfasalazine, leflunomide, cyclosporine, azathioprine, cyclophosphamide, mycophenolate mofetil, 6-thioguanine, acitretin, d-penicillamine, and the following gold preparations: auranofin, myochrysine, or solganol.
A total of 267 study subjects developed incident diabetes. The incidence was highest among patients who were taking nonbiologic DMARDs.
Patients taking a TNF inhibitor or hydroxychloroquine showed a reduced risk of diabetes, compared with patients taking any other agents. After accounting for the effects of potentially confounding factors such as patient age, sex, and several clinical variables, investigators found that the hazard ratios for diabetes were 0.62 for TNF inhibitors and 0.54 for hydroxychloroquine, compared with the nonbiologic DMARDs, Dr. Solomon and his colleagues said (JAMA 2011;305:2525-31).
"These findings held up across a variety of sensitivity analyses," they added.
"Taken in the context of prior research, [our] study supports the potential role for systemic immunosuppression in prevention and control of diabetes. If future studies show this convincingly, systemic immunosuppression in such situations would be predicated on a favorable risk-benefit profile."
For example, the benefit of immunosuppression may outweigh the risk in a patient with a systemic rheumatic disease for which a DMARD is already indicated. But immunosuppression may not outweigh the risk in a patient who already has diabetes and is prone to infection.
The investigators emphasized that this was an observational epidemiologic study without randomized-treatment assignment, so causation cannot be inferred. "It is possible that patients receiving a TNF inhibitor or hydroxychloroquine were different from the reference group of other nonbiologic DMARD users in ways that went unmeasured, such as body mass index, exercise participation, family history, or disease severity," they noted.
They added that the findings warrant confirmation in a randomized, controlled trial to test "the ability of these agents to prevent diabetes among participants with systemic inflammatory disorders."
This study was supported by Amgen. Dr. Solomon reported ties to Abbott, Amgen, Bristol-Myers Squibb, and Pfizer, and his associates reported ties to numerous industry sources.