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April 11, 2012Article

Survival in MS

A randomized cohort study 21 years after the start of the pivotal IFNβ-1b trial

D.S. Goodin, A.T. Reder, G.C. Ebers, G. Cutter, M. Kremenchutzky, J. Oger, D. Langdon, M. Rametta, K. Beckmann, T.M. DeSimone, V. Knappertz
First published April 11, 2012, DOI: https://doi.org/10.1212/WNL.0b013e3182535cf6
D.S. Goodin
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A.T. Reder
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G.C. Ebers
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G. Cutter
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M. Kremenchutzky
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J. Oger
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D. Langdon
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M. Rametta
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K. Beckmann
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T.M. DeSimone
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V. Knappertz
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Citation
Survival in MS
A randomized cohort study 21 years after the start of the pivotal IFNβ-1b trial
D.S. Goodin, A.T. Reder, G.C. Ebers, G. Cutter, M. Kremenchutzky, J. Oger, D. Langdon, M. Rametta, K. Beckmann, T.M. DeSimone, V. Knappertz
Neurology Apr 2012, WNL.0b013e3182535cf6; DOI: 10.1212/WNL.0b013e3182535cf6

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Abstract

Objective: To examine the effects of interferon beta (IFNβ)-1b on all-cause mortality over 21 years in the cohort of 372 patients who participated in the pivotal randomized clinical trial (RCT), retaining (in the analysis) the original randomized treatment-assignments.

Methods: For this randomized long-term cohort study, the primary outcome, defined before data collection, was the comparison of all-cause mortality between the IFNβ-1b 250 μg and placebo groups from the time of randomization through the entire 21-year follow-up interval (intention-to-treat, log-rank test for Kaplan-Meier survival curves). All other survival outcomes were secondary.

Results: After a median of 21.1 years from RCT enrollment, 98.4% (366 of 372) of patients were identified, and, of these, 81 deaths were recorded (22.1% [81 of 366]). Patients originally randomly assigned to IFNβ-1b 250 μg showed a significant reduction in all-cause mortality over the 21-year period compared with placebo (p = 0.0173), with a hazard ratio of 0.532 (95% confidence interval 0.314–0.902). The hazard rate of death at long-term follow-up by Kaplan-Meier estimates was reduced by 46.8% among IFNβ-1b 250 μg–treated patients (46.0% among IFNβ-1b 50 μg–treated patients) compared with placebo. Baseline variables did not influence the observed treatment effect.

Conclusions: There was a significant survival advantage in this cohort of patients receiving early IFNβ-1b treatment at either dose compared with placebo. Near-complete ascertainment, together with confirmatory findings from both active treatment groups, strengthens the evidence for an IFNβ-1b benefit on all-cause mortality.

Classification of Evidence: This study provides Class III evidence that early treatment with IFNβ-1b is associated with prolonged survival in initially treatment-naive patients with relapsing-remitting multiple sclerosis.

  • Received June 8, 2011.
  • Accepted December 14, 2011.
  • Copyright © 2012 by AAN Enterprises, Inc.

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