From the Journals

RA-BEAM trial shows that baricitinib improves RA symptoms, slows joint damage


 

FROM THE NEW ENGLAND JOURNAL OF MEDICINE

Oral baricitinib, when added to standard rheumatoid arthritis treatment, improved symptoms and slowed the progression of joint damage, compared with both placebo and adalimumab, according to a report published online Feb. 15 in the New England Journal of Medicine.

Dr. Peter C. Taylor

Dr. Peter C. Taylor

The study participants were randomly assigned in a double-blind fashion to receive 4 mg of oral baricitinib once per day (487 patients), 40 mg of subcutaneous adalimumab every other week (330 patients), or matching placebo (488 patients), and were followed at 281 medical centers in 26 countries. Nearly all were also receiving background therapy with methotrexate, plus stable doses of conventional synthetic DMARDs, NSAIDs, analgesics, or glucocorticoids (10 mg or less of prednisone or the equivalent per day) at the discretion of their treating physicians.

The primary efficacy endpoint – the proportion of patients at week 12 who showed a response of 20% or more according to American College of Rheumatology criteria (ACR20) – was 70% for baricitinib, compared with 40% for placebo. Baricitinib also was superior to placebo regarding all the major secondary efficacy endpoints of the study, including scores on the Health Assessment Questionnaire–Disability Index; results on the Disease Activity Score for 28 joints using high-sensitivity C-reactive protein (DAS28-CRP); remission according to the Simplified Disease Activity Index criteria; and the patients’ daily diary reports on duration and severity of morning joint stiffness, worst level of tiredness, and worst level of pain.

In addition, baricitinib was “considered to be significantly superior to adalimumab” according to the ACR20 (61% for adalimumab) and the DAS28-CRP responses at week 12. Both baricitinib and adalimumab were associated with significant reductions in the radiographic progression of structural joint damage, compared with placebo, at week 24 and week 52, the investigators reported (N Engl J Med. 2017;376:652-62).

Regarding safety outcomes, adverse events including infections were more frequent with baricitinib and adalimumab than with placebo, as were decreases in neutrophil counts, increases in aminotransferase and creatinine levels, and increases in low-density lipoprotein cholesterol levels. At 1 year, three patients in the baricitinib group and two in the adalimumab group discontinued treatment because of liver abnormalities.

Baricitinib is currently under consideration for approval by the U.S. Food and Drug Administration and was approved for marketing in the European Union on Feb. 13.

The RA-BEAM trial was supported by Eli Lilly and Incyte. Dr. Taylor reported receiving personal fees from Eli Lilly, and he and his associates reported ties to numerous other industry sources.

Recommended Reading

Infliximab biosimilar posts mostly reassuring data in Norway’s NOR-SWITCH study
MDedge Family Medicine
Breast milk doesn’t contain meaningful levels of certolizumab pegol
MDedge Family Medicine
Prenatal exposure to TNF inhibitors does not increase infections in newborns
MDedge Family Medicine
Tocilizumab raises cholesterol, but not cardiovascular events
MDedge Family Medicine
Medicare payments set for infliximab biosimilar Inflectra
MDedge Family Medicine
All systemic steroid guidelines for RA offer little guidance
MDedge Family Medicine
FDA opens abbreviated approval pathway for interchangeable biosimilars
MDedge Family Medicine
Hydroxychloroquine dosing guidelines have little impact in clinical practice
MDedge Family Medicine
Perioperative infliximab does not increase serious infection risk
MDedge Family Medicine
ACR guidelines on HBV screening called inadequate
MDedge Family Medicine

Related Articles