Lily Jung Henson, MD
,
Swedish Issaquah, Issaquah, WA, USA, Issaquah, WA
Douglas L Arnold, MD
,
Montreal Neurological Institute, McGill University, and NeuroRx Research, Montreal, Quebec, Canada, Montreal, QC, Canada
Jeffrey A Cohen, MD
,
Mellen Center, Cleveland Clinic, Cleveland, OH, USA, Cleveland, OH
Alasdair J Coles, MD
,
University of Cambridge, Cambridge, UK, Cambridge, United Kingdom
Christian Confavreux, MD
,
University Claude Bernard, Lyon, France, Lyon, France
Edward J Fox, MD
,
MS Clinic of Central Texas, Round Rock, TX, USA, Round Rock, TX
Hans-Peter Hartung, MD
,
Heinrich-Heine University, Dusseldorf, Germany, Dusseldorf, Germany
Eva Havrdova, MD, PhD
,
Department of Neurology, First Faculty of Medicine, Charles University in Prague, Prague, Czech Republic, Prague, Czech Republic
Krzysztof Selmaj, MD, PhD
,
Medical University of Lodz, Lodz, Poland, Lodz, Poland
Howard L Weiner, MD
,
Brigham and Women's Hospital Center for Neurologic Diseases, Boston, MA, USA, Boston, MA
Tamara A Miller, MD
,
Advanced Neurology of Colorado, Ft Collins, CO, USA, Ft Collins, CO
Cary L Twyman, MD
,
Associates in Neurology PSC, Lexington, KY, USA, Lexington, KY
Stephen L Lake, ScD
,
Genzyme, Cambridge, MA, USA, Cambridge, MA
David H Margolin, MD
,
Genzyme, Cambridge, MA, USA, Cambridge, MA
Michael A Panzara, MD
,
Genzyme, Cambridge, MA, USA, Cambridge, MA
Alastair Compston, MD
,
University of Cambridge, Cambridge, UK, Cambridge, United Kingdom
Background: In CARE-MS II, alemtuzumab reduced the relapse rate over 2 years compared with subcutaneous interferon beta-1a (SC IFNB-1a) (0.26 vs. 0.52; 49% reduction;
P < 0.0001) in active RRMS patients who had experienced disease activity on prior therapy.
Objectives: Evaluate the effects of alemtuzumab on relapse rate over time in the CARE-MS II study.
Methods: Active RRMS patients who had relapsed on prior therapy were randomized to receive alemtuzumab 12 mg intravenously on 5 days at study start and on 3 days 1 year later or SC IFNB-1a 44 µg 3-times weekly. Relapse events were required to last ≥48 h, required objective signs as assessed by blinded raters, and were adjudicated by an independent committee.
Results: Alemtuzumab’s superior effect on relapse reduction was statistically significant (P = 0.046) within 4 months of initiating treatment and was maintained throughout the study period. Compared with IFNB-1a, alemtuzumab reduced the relapse rate by 54% in Year 1 (P < 0.0001) and 41% in Year 2 (i.e., Months 12 to 24) (P = 0.0017). Percentage of patients experiencing relapse in the alemtuzumab group versus the IFNB-1a group were 12% vs 29% through Month 6, 24% vs 43% through Month 12, and 35% vs 51% through Month 24. Analysis of cumulative monthly relapses among patients receiving alemtuzumab showed that its effect on relapse rate was consistent throughout the 24 months of the study.
Conclusions: Alemtuzumab suppressed relapses more effectively than high-dose, high-frequency SC IFNB-1a in active RRMS patients who had experienced disease activity on previous therapy. The greater effect of alemtuzumab on relapse rate became significant within 4 months of treatment initiation and was durable throughout the 2-year study period.
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