ACR Study: Belimumab Improves CLE Too
Belimumab, a monoclonal antibody that inhibits B-cell activation, is approved for SLE but less is known about its use in CLE, including the time to response after starting the drug.
The B-cell inhibitor belimumab significantly improved cutaneous lupus erythematosus (CLE) whether or not patients also had systemic lupus erythematosus (SLE), according to research presented at ACR Convergence 2022, the American College of Rheumatology’s annual meeting,
Belimumab, a monoclonal antibody that inhibits B-cell activation, is approved for SLE but less is known about its use in CLE, including the time to response after starting the drug.
Researchers undertook this meta-analysis to examine the efficacy of belimumab and the time to response in CLE patients with or without SLE.
After a comprehensive manual search of more than 700 interventional and observational studies, the researchers identified six blinded interventional studies to include in the meta-analysis, where belimumab was compared to the standard of care, such as conventional disease-modifying anti-rheumatic drugs (DMARDs) or prednisone plus hydroxychloroquine. Included studies were homogenous, with a low risk of bias.
The primary outcome was clinical response at 52 weeks in belimumab users compared to non-users. Clinical response was defined as a decrease in skin manifestations from a baseline British Isles Lupus Assessment Group (BILAG) score of A or B to a BILAG score of B-E. The BILAG index is a validated measure of disease activity in SLE.
The researchers calculated the pooled odds ratio for each consecutive four-week interval to find the clinical response time and the time to sustained response in belimumab users compared to nonusers. They also pooled the odds of skin flares at one year.
The resulting analysis showed the odds of clinical response at 52 weeks were 44 percent higher in patients using belimumab. Clinical response was first noted 20 weeks after staring the drug, with a sustained clinical response peaking at one year. Patients using belimumab also had a 49 percent lower risk of severe skin flares.
“Our study is the first meta-analysis of belimumab’s efficacy in CLE and highlights that it is an effective adjunct therapy for patients with CLE as a primary manifestation of SLE,” says Shivani Garg, MD, MS, Assistant Professor at the University of Wisconsin School of Medicine and Public Health and the study’s lead author, in a news release. “The study also highlights that belimumab can take at least 20 weeks to achieve a sustained clinical response in patients with CLE, so it should not be prematurely discontinued in these patients.”
Dr. Garg also points to findings showing that belimumab users have a nearly 50 percent lower chance of a severe cutaneous flare compared to nonusers.
The study did not examine the comparative efficacy of belimumab in different subtypes of CLE, but Dr. Garg says it “lays a foundation for future studies across CLE subtypes.”