PMID- 17692727
OWN - NLM
STAT- MEDLINE
DCOM- 20070925
LR  - 20151119
IS  - 0149-2918 (Print)
IS  - 0149-2918 (Linking)
VI  - 29
IP  - 6
DP  - 2007 Jun
TI  - Immunogenicity and tolerability of an investigational formulation of 
      interferon-beta1a: 24- and 48-week interim analyses of a 2-year, single-arm, 
      historically controlled, phase IIIb study in adults with multiple sclerosis.
PG  - 1128-45
AB  - BACKGROUND: RNF (Rebif New Formulation, Merck Serono International S.A., Geneva, 
      Switzerland), a formulation of interferon-beta1a (IFN-beta1a) without human- or 
      animal-derived components, is currently under investigation. It was developed 
      with the aim of maximizing the treatment benefit for patients with multiple 
      sclerosis (MS) by improving injection tolerability and reducing the development 
      of neutralizing antibodies (NAbs). OBJECTIVE: This paper reports the results of 
      planned 24- and 48-week interim analyses comparing immunogenicity and 
      tolerability data from an ongoing study of RNF with historical-control data for 
      the currently approved formulation of IFN-beta1a from the EVIDENCE (EVidence of 
      Interferon Dose-response: European North American Comparative Efficacy) study. 
      METHODS: Patients in the 96-week, multicenter, singlearm, Phase IIIb RNF study 
      received 44 microg/0.5 mL SC tiw; patients in the EVIDENCE study received an 
      identical regimen of the currently approved formulation of IFN-beta1a. Criteria 
      for inclusion in the RNF study were age between 18 and 60 years, an Expanded 
      Disability Status Scale (EDSS) score <6.0, and a diagnosis of relapsing MS 
      (McDonald criteria). Criteria for inclusion in the EVIDENCE study were age 
      between 18 and 55 years, an EDSS score of 0 to 5.5, and a diagnosis of clinically 
      definite relapsing-remitting MS (Poser criteria). Patients in both studies were 
      treatment naive. Both studies used the same cytopathic-effect assay for NAbs to 
      assess immunogenicity; patients who had NAb titers >or=20 neutralizing units 
      (NU)/mL were considered NAb+. The primary end point was to compare the 
      proportions of NAb+ patients in the RNF study and the historical data. 
      Comparisons were descriptive and used exact 95% CIs. Safety analyses included 8 
      prespecified adverse events (AEs) of interest. RESULTS: Baseline demographic 
      characteristics were well balanced between the RNF (N = 260) and EVIDENCE (N = 
      339) studies, except that patients in the RNF study were slightly younger (median 
      age, 34.0 vs 39.0 years, respectively), and a few had secondary progressive MS (n 
      = 6) or progressive relapsing MS (n = 1). At week 48, 87.3% of patients in the 
      RNF study remained on treatment. The incidence of the prespecified AEs of 
      interest in the RNF and EVIDENCE studies was as follows: flu-like symptoms (70.8% 
      and 48.1%, respectively), injection-site reactions (29.6% and 83.8%), hepatic 
      disorders (13.1% and 16.8%), cytopenia (9.6% and 11.8%), depression and suicidal 
      ideation (5.8% and 19.8%), skin rashes (5.4% and 12.1%), hypersensitivity 
      reactions (5.4% and 3.2%), and thyroid disorders (2.3% and 5.0%). Overall, the 
      majority (96.9%) of AEs in the RNF study were mild (69.5%) or moderate (27.5%) in 
      severity. The proportions of patients in the RNF and EVIDENCE studies with NAbs 
      at both 24 and 48 weeks were 2.5% (95% CI, 0.9-5.5) and 14.3% (95% CI, 
      10.7-18.6), respectively; the proportions with NAbs at week 48 only were 13.9% 
      (95% CI, 9.9-18.7) and 24.4% (95% CI, 19.9-29.4). The proportions of NAb+ 
      patients with high NAb titers (>1000 NU/mL) at week 48 were 11.1% in the RNF 
      study and 19.5% in the EVIDENCE study. CONCLUSIONS: The results of these interim 
      analyses suggest that RNF had an improved overall tolerability and safety profile 
      and a lower immunogenic potential compared with the approved IFN-beta1a 
      formulation assessed in the EVIDENCE study. Two-year results from the RNF study 
      are anticipated before the end of 2007.
FAU - Giovannoni, Gavin
AU  - Giovannoni G
AD  - Neuroimmunology Unit, Institute of Cell and Molecular Science, Queen Mary 
      University London, London, United Kingdom.
FAU - Barbarash, Olga
AU  - Barbarash O
FAU - Casset-Semanaz, Florence
AU  - Casset-Semanaz F
FAU - Jaber, Amer
AU  - Jaber A
FAU - King, John
AU  - King J
FAU - Metz, Luanne
AU  - Metz L
FAU - Pardo, Gabriel
AU  - Pardo G
FAU - Simsarian, James
AU  - Simsarian J
FAU - Sorensen, Per Soelberg
AU  - Sorensen PS
FAU - Stubinski, Bettina
AU  - Stubinski B
CN  - RNF Study Group
LA  - eng
PT  - Clinical Trial, Phase III
PT  - Journal Article
PT  - Multicenter Study
PT  - Research Support, Non-U.S. Gov't
PL  - United States
TA  - Clin Ther
JT  - Clinical therapeutics
JID - 7706726
RN  - 0 (Immunologic Factors)
RN  - 77238-31-4 (Interferon-beta)
RN  - XRO4566Q4R (Interferon beta-1a)
SB  - IM
MH  - Adolescent
MH  - Adult
MH  - Chemistry, Pharmaceutical
MH  - Dose-Response Relationship, Drug
MH  - Europe
MH  - Female
MH  - Humans
MH  - Immunologic Factors/adverse effects/immunology/*therapeutic use
MH  - Interferon beta-1a
MH  - Interferon-beta/adverse effects/immunology/*therapeutic use
MH  - Male
MH  - Middle Aged
MH  - Multiple Sclerosis/*drug therapy/immunology
MH  - North America
MH  - Prospective Studies
MH  - Single-Blind Method
MH  - Time Factors
MH  - Treatment Outcome
EDAT- 2007/08/19 09:00
MHDA- 2007/09/26 09:00
CRDT- 2007/08/19 09:00
PHST- 2007/04/18 00:00 [accepted]
PHST- 2007/08/19 09:00 [pubmed]
PHST- 2007/09/26 09:00 [medline]
PHST- 2007/08/19 09:00 [entrez]
AID - S0149-2918(07)00161-0 [pii]
AID - 10.1016/j.clinthera.2007.06.002 [doi]
PST - ppublish
SO  - Clin Ther. 2007 Jun;29(6):1128-45. doi: 10.1016/j.clinthera.2007.06.002.