All doses of tirzepatide consistently reduced body weight in women and men, but women experienced greater weight loss, according to post hoc research presented at this year's Annual Meeting of the European Association for the Study of Diabetes.
The post hoc analysis, which included the four SURMOUNT trials, compared tirzepatide with a placebo for up to 72 to 88 weeks in 4,677 adults (2,999 females, 1,678 males) living with obesity, highlighting potential sex differences in the response.
The phase 3 SURMOUNT clinical trials examined the efficacy and safety of tirzepatide versus placebo in people with a BMI of 30kg/m2 and above, or 27kg/m2 with at least one weight-related comorbidity without type 2 diabetes (SURMOUNT-1, 72 weeks), with type 2 diabetes (T2D) (SURMOUNT-2; 72 weeks), and without T2D after a 12-week intensive lifestyle intervention (SURMOUNT-3; 72 weeks from randomization), or after an 88 week intervention (SURMOUNT-4; 36-week open label tirzepatide lead-in and 52 weeks following randomisation).
The post-hoc analyses examined whether the weight-lowering effects of tirzepatide vary according to sex in these trials. All randomised participants (51-71% female) who received at least one dose of the study drug (tirzepatide 5, 10, or 15mg or placebo) were included.
At randomisation, the average body weight and body mass index (BMI) for females vs. males was 99.8 vs. 115.2kg and 38.2 vs. 37.6kg/m2 in SURMOUNT-1; 94.8 vs. 106.8kg and 36.7 vs. 35.4kg/m2 in SURMOUNT-2; 95.4 vs. 112.9kg and 35.8 vs. 36.1kg/m2 in SURMOUNT-3; and 79.6 vs. 98.6kg and 30.1 vs. 31.4kg/m2 in SURMOUNT-4, respectively.
The researchers examined the average percentage change in body weight from randomiSation to week 72 (SURMOUNT-1, -2, and -3) or to week 52 (SURMOUNT-4) by sex, as well as assessing the sex differences in the proportion of participants achieving weight reduction targets of at least 5%, 10% and 15%. The analyses found that across all trials, tirzepatide treatment was associated with significant weight reduction compared to placebo, regardless of sex, ranging from11.5% to -27.6% in females and -8.8% to -18.9% in males.
Additionally, the odds of achieving weight reduction targets were significantly higher with tirzepatide treatment, compared with placebo in both males and females. Nevertheless, female participants achieved greater reductions in weight with tirzepatide treatment (up to 24.6%), compared to male participants (up to 18.1%) across all trials.
Similar proportions of males and females achieved the body weight reduction thresholds of at least 5%, 10% and 15% with tirzepatide treatment in SURMOUNT-1, -2, and -4, or achieved the 15% target in SURMOUNT-3.
However, in the SURMOUNT 3 trial involving adults without T2D, tirzepatide-treated females were significantly more likely to achieve a body weight reduction of at least 5% and 10% than tirzepatide-treated males. The safety profile was broadly similar by sex, but a numerically higher incidence of nausea and vomiting was noted in females.
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