Table 2.

Efficacy outcomes from key registration trials

	TEMSO		TOWER
	Teriflunomide 14 mg (n = 358)	Placebo (n = 363)	Teriflunomide 14 mg (n = 370)	Placebo (n = 388)
Annualized relapse rate	0.37	0.54	0.32	0.50
Relative reduction vs. placebo (%)	31.5***	–	36.0****	–
Patients remaining relapse free at week 108 (%)	56.5	45.6	57.1	46.8
Hazard ratio vs. placebo	0.72**	–	0.63****	–
Patients with 3-month sustained disability progression at week 108 (%)	20.2	27.3	15.8	19.7
Hazard ratio vs. placebo	0.70*	–	0.68*	–
Risk reduction vs. placebo (%)	30.0	–	32.0	–
Patients free of MRI activitya at week 108 (%)	37.6****b OR 2.26 (1.61–3.17)	21.1	–	–
Patients with no evidence of disease activityc at week 108 (%)	21.2***b OR 2.06 (1.35–3.13)	11.6	–	–
Change from baseline in total lesion volume (ml)d at week 108	0.72	2.21	–	–
Relative reduction vs. placebo (%)	67.0***	–	–	–
Mean number of T1 Gd-enhancing lesions per scan	0.38	1.18	–	–
Change relative to placebo	−0.80****	–	–	–
Number of unique active lesions per scan	0.75	2.46	–	–
Relative reduction vs. placebo (%)	69.0****	–	–	–

Data in parentheses are 95 % confidence intervals

Gd gadolinium, MRI magnetic resonance imaging, OR odds ratio

* p < 0.05, ** p < 0.01, *** p < 0.001, **** p < 0.0001

^aMRI activity was defined as no Gd-enhancing T1 lesions and no new/enlarging T2 lesions. Evaluable patients must have at least one valid MRI scan for assessment over the study duration; Placebo, n = 346; 14 mg, n = 340

^bData on file

^cNo evidence of disease activity was defined as no Gd-enhancing T1 lesions, no new/enlarging T2 lesions, no confirmed clinical relapse, and no 3-month sustained disability progression. Evaluable patients must have both valid MRI and clinical activity assessments over the study duration; Placebo, n = 346; 14 mg, n = 340

^dTotal volume of all abnormal brain tissue and calculated as the sum of the total volume of T2 lesion component and T1 hypointense lesion component