Physician Greater Houston Diabetes & Endocrinology Center Humble, Texas, United States
Background Glucagon Like Peptide -1 (GLP-1) receptor agonists are widely used for managing obesity and improving glycemic control in diabetes. Weight loss of 5-10% reduces obesity-related complications and improves quality of life, while greater weight loss with GLP-1 RAs demonstrated 20% reduction in major cardiovascular events in non-diabetic patients (1). Recent evidence shows that patients with hypothyroidism who lose more than 5 lb after starting a GLP-1 medication experience an average 0.36 - 0.55 mIU/L reduction in TSH levels.
Methods: A retrospective cohort study of 50 non-diabetic adults with obesity (BMI ≥30 kg/m²) on GLP-1 receptor agonists was conducted at an outpatient clinic. After screening 200 patients, 50 met inclusion criteria (HbA1c < 6.5%, normal thyroid function or treated hypothyroidism with stable thyroid function, no concurrent anti-obesity medications). Patients on semaglutide (n=25, up to 2.4 mg weekly) were compared to those on tirzepatide (n=25, up to 15 mg weekly). The primary outcome was mean weight change at 12 months. Secondary outcomes included BMI reduction, HbA1c change, TSH suppression, and adverse events.
Results: Tirzepatide demonstrated superior weight loss compared to semaglutide (mean weight loss: 37.1 lb vs 20.2 lb; mean BMI reduction: -6.13 kg/m² vs -3.39 kg/m²; p< 0.001). Mean HbA1c reduction was comparable (-0.31% vs -0.28%). TSH reduction occurred proportionally to weight loss in both groups, with greater reductions observed in trizepatide cohort (mean -0.8 to -1.3 mIU/L) compared with semaglutide cohort (mean -0.25 to -0.55 mIU/L), with stable free T4 levels. Treatment persistence was markedly higher with tirzepatide (67%) versus semaglutide (13%). Insurance/cost barriers caused discontinuation in 47% of semaglutide versus 21% of tirzepatide patients. Metformin co-administration was present in 33% of patients. GI-related discontinuation was lower with tirzepatide (8%) versus semaglutide (12%). Weight regain after discontinuation was universal and rapid (50-67% regain within 3-6 months) in both groups, emphasizing the need for long -term management strategies.
Conclusion: In obese non-diabetic adults, tirzepatide produced significantly greater weight loss and superior treatment persistence compared to semaglutide at 12 months. TSH suppression reflected physiological adaptation to weight loss rather than drug-induced thyroid dysfunction. Insurance barriers were the primary driver of treatment failure, highlighting the need for improved access to effective therapies.
References: 1. Rodriguez, P. J., Goodwin Cartwright, B. M., Gratzl, S., et al. (2024). Semaglutide vs tirzepatide for weight loss in adults with overweight or obesity. JAMA Internal Medicine, 184(9), 1056-1064.
*Unless otherwise noted, all abstracts presented at ENDO must not be released to the press or the public until the date and time of presentation. For oral presentations, the abstracts are embargoed until the session begins. The Endocrine Society reserves the right to lift the embargo on specific abstracts that are selected for promotion prior to or during ENDO.*
.jpg)
.jpg)