Brain magnetic resonance imaging at 1 year demonstrating 1 contrast-enhancing lesion or 2 T2 lesions had the same implication for future disease as 1 clinical relapse.
After initiating disease-modifying therapy (DMT) in multiple sclerosis (MS), assessment of treatment response is critical. Early disease activity increases the risk for later disability progression. The European Medicines Agency (EMA) clinical guidelines for prompt consideration of so-called second-line agents (i.e., natalizumab, fingolimod) include a clinical relapse in the year following DMT initiation, accompanied by either a contrast-enhancing lesion (CEL) or ≥9 T2 lesions at baseline. However, the impact of subclinical magnetic resonance imaging (MRI) lesions has not been addressed sufficiently.
Now, researchers have evaluated the relation between MRI lesion count thresholds during treatment year 1 and 4-year outcomes. A total of 370 pa…
Reviewing Author
DisclosuresConsultant/Advisory BoardAlexion Pharmaceuticals; Amgen; Astoria; Biogen; Bristol Myers Squibb; Celltrion; Genentech; Hoffmann-La Roche; Genzyme; EMD Serono; Immpact-Bio; Immunic Therapeutics; Kyverna; Lundbeck; Novartis; Sandoz; TG Therapeutics
Grant/Research SupportNational Institutes of Health; National Multiple Sclerosis Society; U.S. Department of Defense
Leadership Positions in Professional SocietiesConsortium of Multiple Sclerosis Centers (Treasurer)
DisclosuresConsultant/Advisory BoardAlexion Pharmaceuticals; Amgen; Astoria; Biogen; Bristol Myers Squibb; Celltrion; Genentech; Hoffmann-La Roche; Genzyme; EMD Serono; Immpact-Bio; Immunic Therapeutics; Kyverna; Lundbeck; Novartis; Sandoz; TG Therapeutics
Grant/Research SupportNational Institutes of Health; National Multiple Sclerosis Society; U.S. Department of Defense
Leadership Positions in Professional SocietiesConsortium of Multiple Sclerosis Centers (Treasurer)