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. 2012 May 16;4:81–103. doi: 10.4137/JCNSD.S6692

Table 4.

Efficacy of New and Emerging Oral Therapies.

Therapy Pivotal Trials Design Patients Key Endpoints
Fingolimod TRANSFORMS 1 year RRMS ↓ ARR (0.5mg = 0.16, 1.25mg = 0.2, IFN = 0.33)
↓ New or enlarged T2 lesions ( high and low dose fingolimod arms)
No difference in 3-month disability progression
Phase III
Double-blind
Double dummy
Randomized 1:1:1 of 0.5mg, 1.25mg, or qwk IM IFN beta-1a
FREEDOMS 2 year RRMS ↓ ARR (0.5mg = 0.18, 1.25mg = 0.16, placebo = 0.4)
Absence of 3-month disability progression (0.5mg = 82.3%, 1.25mg = 83.4%, placebo 75.9%)
↓ Number of Gd+ lesions (0.5mg = 0.2, 1.25mg = 0.2, placebo = 1.1)
↓ Number of new/enlarged T2 lesions (0.5mg = 2.5, 1.25mg = 2.5, placebo = 9.8)
↓ Volume of T1-hypointense lesions (0.5mg = 8.8, 1.25mg = 12.2, Placebo = 50.7)
↓ Brain atrophy (0.5mg = −0.37, 1.25mg = −0.42, placebo = 0.81)
Phase III
Double-blind
Randomized 1:1:1 or 0.5mg, 1.25mg, or placebo
Teriflunomide TEMSO 2 year RRMS, SPMS, PPMS ↓ ARR (7mg = 31.2%, 14mg = 31.5%)
↓ Disability progression in 14mg group
↓ Decreased T2 lesion volume (7mg = 1.31, 14mg = 0.72, placebo = 2.21)
↓ Decreased Gd+ lesions (7mg = 0.57, 14mg = 0.26, Placebo = 1.33)
↓ Unique active lesions (7mg = 1.29, 14mg=0.75, Placebo = 2.46)
↓ Volume of T1 hypointense lesions in 14mg
No difference in brain atrophy among groups
Phase III
Double-blind
Randomized 1:1:1 of 7mg, 14mg, or placebo
TENERE 2 year No difference in risk of treatment failure
No difference in ARR
(7mg = 0.410, 14mg = 0.259, IFN = 0.216)
Phase III
Rater-blinded
Randomized 1:1:1 of 7mg, 14mg, or tiw IFN-β-1a
BG-12 DEFINE 2 year ↓ Risk of relapse (bid = 49%, tid = 50%)
↓ ARR (bid = 53%, tid = 48%)
↓ Risk of disability progression (bid=38%, tid=34%)
Phase III
Double-blind
Randomized 1:1:1 bid, tid, or placebo
CONFIRM 2 year RRMS ↓ARR (bid=44%, tid = 51%, GA = 29%)
↓New/enlarging T2 lesions (bid = 71%, tid = 73%, GA = 54%)
↓ New T1 hypointense lesions (bid=57%, tid=65%, GA = 41%)
↓ Proportion of patientsrelapsing (bid=34%, tid = 45%, GA = 29%)
No difference in disability progression among groups
Phase III
Double-blind
Randomized 1:1:1:1 bid, tid, GA, or placebo
Laquinimod ALLEGRO 2 year RRMS ARR ↓23%
↓ New/enlarging T2 lesions
↓ New T1 hypointense lesions
↓ Brain atrophy
Disability progression ↓36%
Brain atrophy ↓32.8%
Rate of severe relapses (↓27%
Phase III
Randomized 1:1 of 0.6mg or placebo
BRAVO 2 year RRMS Adjusted ARR (0.6mg = 0.29, placebo = 0.37, IFN-β-1a = 0.27)
↓ Risk of disability progression Brain atrophy
↓27.5%
Phase III
Double-blind
Randomized 1:1:1 of 0.6mg, placebo, or qwk IM IFN-β-1a