TY - JOUR
T1 - Randomized controlled trial of atorvastatin in clinically isolated syndrome
T2 - The STAyCIS study
AU - ITN STAyCIS Study Group
AU - ITN020AI Study Management Team
AU - Waubant, E.
AU - Pelletier, D.
AU - Mass, M.
AU - Cohen, J. A.
AU - Kita, M.
AU - Cross, A.
AU - Bar-Or, A.
AU - Vollmer, T.
AU - Racke, M.
AU - Stüve, O.
AU - Schwid, S.
AU - Goodman, A.
AU - Kachuck, N.
AU - Preiningerova, J.
AU - Weinstock-Guttman, B.
AU - Calabresi, P. A.
AU - Miller, A.
AU - Mokhtarani, M.
AU - Iklé, D.
AU - Murphy, S.
AU - Kopetskie, H.
AU - Ding, L.
AU - Rosenberg, E.
AU - Spencer, C.
AU - Zamvil, S. S.
AU - Bourdette, D.
AU - Egan, R.
AU - Stone, L.
AU - Elliott, M.
AU - Parks, B. J.
AU - Campagnolo, D.
AU - Stüve, O.
AU - Frohman, E.
AU - Segal, B.
AU - Weiner, L.
AU - Carrithers, M.
AU - Kerr, D.
AU - Lublin, F.
AU - Sayre, P.
AU - Hayes, D.
AU - Gao, W.
AU - Adah, S.
AU - Neuenburg, J.
AU - Bromstead, C.
AU - Olinger, L.
AU - Mullen, B.
AU - Jamison, R.
AU - Speth, K.
AU - Saljooqi, K.
AU - Phan, P.
N1 - Funding Information:
This research was performed as a project of the Immune Tolerance Network (ITN020AI, ITN contract number N01-AI-15416) , a clinical research consortium sponsored by the National Institute of Allergy and Infectious Diseases. Pfizer provided atorvastatin, placebo, and grant support. Biogen Idec provided IFNβ-1a IM and grant support. E.W. is also supported by the Nancy Davis Foundation. S.S.Z. was also supported for this study by the National Institutes of Health (RO1 AI059709) and the Maisin Foundation.
Funding Information:
The authors thank members of the Central MRI unit (Dr. Okuda and project coordinator Alan Evangelista), site coordinators, and patients for their contributions to this study; and Dr. Gary Cutter for discussions. The centralized MRI reading was performed by the Advanced Imaging in Multiple Sclerosis (AIMS) Laboratory at UCSF (Dr. Daniel Pelletier, Director). The Data Safety Monitoring Board was sponsored by NIAID, and provided clinical, statistical, and ethical support.
PY - 2012/4/10
Y1 - 2012/4/10
N2 - Objective: To test efficacy and safety of atorvastatin in subjects with clinically isolated syndrome (CIS). Methods: Subjects with CIS were enrolled in a phase II, double-blind, placebo-controlled, 14-center randomized trial testing 80mgatorvastatin on clinical and brain MRI activity. Brain MRIs were performed quarterly.Theprimary endpoint (PEP)wasdevelopmentof≥3newT2lesions, oroneclinical relapse within 12months. Subjects meeting the PEP were offered additional weekly interferonβ-1a (IFNβ-1a). Results: Due to slow recruitment, enrollment was discontinued after 81 of 152 planned subjects with CIS were randomized and initiated study drug. Median (interquartile range) numbers of T2 and gadolinium-enhancing (Gd) lesions were 15.0 (22.0) and 0.0 (0.0) at baseline. A total of 53.1% of atorvastatin recipients (n = 26/49) met PEP compared to 56.3% of placebo recipients (n = 18/32) (p = 0.82). Eleven atorvastatin subjects (22.4%) and 7 placebo subjects (21.9%) met the PEP by clinical criteria. Proportion of subjects who did not develop new T2 lesions up to month 12 or to starting IFNβ-1a was 55.3% in the atorvastatin and 27.6% in the placebo group (p = 0.03). Likelihood of remaining free of new T2 lesions was significantly greater in the atorvastatin group compared with placebo (odds ratio [OR] = 4.34, p = 0.01). Likelihood of remaining free of Gd lesions tended to be higher in the atorvastatin group (OR=2.72, p=0.11). Overall, atorvastatin was well tolerated. No clear antagonistic effect of atorvastatin plus IFNβ-1a was observed on MRI measures. Conclusion: Atorvastatin treatment significantly decreased development of new brain MRI T2 lesion activity, although it did not achieve the composite clinical and imaging PEP. Classification of Evidence: This study provided Class II evidence that atorvastatin did not reduce the proportion of patients with CIS meeting imaging and clinical criteria for starting immunomodulating therapy after 12 months, compared to placebo. In an analysis of a secondary endpoint (Class III), atorvastatin was associated with a reduced risk for developing new T2 lesions.
AB - Objective: To test efficacy and safety of atorvastatin in subjects with clinically isolated syndrome (CIS). Methods: Subjects with CIS were enrolled in a phase II, double-blind, placebo-controlled, 14-center randomized trial testing 80mgatorvastatin on clinical and brain MRI activity. Brain MRIs were performed quarterly.Theprimary endpoint (PEP)wasdevelopmentof≥3newT2lesions, oroneclinical relapse within 12months. Subjects meeting the PEP were offered additional weekly interferonβ-1a (IFNβ-1a). Results: Due to slow recruitment, enrollment was discontinued after 81 of 152 planned subjects with CIS were randomized and initiated study drug. Median (interquartile range) numbers of T2 and gadolinium-enhancing (Gd) lesions were 15.0 (22.0) and 0.0 (0.0) at baseline. A total of 53.1% of atorvastatin recipients (n = 26/49) met PEP compared to 56.3% of placebo recipients (n = 18/32) (p = 0.82). Eleven atorvastatin subjects (22.4%) and 7 placebo subjects (21.9%) met the PEP by clinical criteria. Proportion of subjects who did not develop new T2 lesions up to month 12 or to starting IFNβ-1a was 55.3% in the atorvastatin and 27.6% in the placebo group (p = 0.03). Likelihood of remaining free of new T2 lesions was significantly greater in the atorvastatin group compared with placebo (odds ratio [OR] = 4.34, p = 0.01). Likelihood of remaining free of Gd lesions tended to be higher in the atorvastatin group (OR=2.72, p=0.11). Overall, atorvastatin was well tolerated. No clear antagonistic effect of atorvastatin plus IFNβ-1a was observed on MRI measures. Conclusion: Atorvastatin treatment significantly decreased development of new brain MRI T2 lesion activity, although it did not achieve the composite clinical and imaging PEP. Classification of Evidence: This study provided Class II evidence that atorvastatin did not reduce the proportion of patients with CIS meeting imaging and clinical criteria for starting immunomodulating therapy after 12 months, compared to placebo. In an analysis of a secondary endpoint (Class III), atorvastatin was associated with a reduced risk for developing new T2 lesions.
UR - http://www.scopus.com/inward/record.url?scp=84860723016&partnerID=8YFLogxK
U2 - 10.1212/WNL.0b013e31824f7fdd
DO - 10.1212/WNL.0b013e31824f7fdd
M3 - Article
C2 - 22459680
AN - SCOPUS:84860723016
SN - 0028-3878
VL - 78
SP - 1171
EP - 1178
JO - Neurology
JF - Neurology
IS - 15
ER -