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Tirzepatide as an innovative treatment strategy in a pre-clinical model of obesity-driven endometrial cancer.

Gynecol Oncol · 2024

Last updated 2026-06-21

In a mouse study, tirzepatide—a drug that targets GLP-1 and GIP receptors—led to a 20.1% weight loss in obese mice and a 16.8% weight loss in lean mice after 4 weeks of treatment. The drug also reduced tumor growth in both groups and improved markers related to metabolism and inflammation. The effects on tumors involved different biological pathways depending on whether the mice were obese or lean.

AI summary of the abstract below.

JournalGynecol Oncol, 2024
Citations24
Relative citation ratio4.25
NIH percentile90
Molecules tirzepatide

Abstract

OBJECTIVE: Interventions that combat obesity and its associated metabolic perturbations may decrease incidence and improve outcomes of endometrial cancer (EC). Potential options for weight loss include pharmacotherapeutic interventions such as tirzepatide, a dual-acting glucagon-like peptide 1 (GLP-1) and gastric inhibitory polypeptide (GIP) receptor agonist. Given this, we explored the anti-obesity and anti-tumorigenic effects of tirzepatide in our pre-clinical mouse model of endometrioid EC. METHODS: Starting at 4 weeks of age, Lkb1p53 mice were fed a low-fat diet vs a high-fat diet to generate a lean or obese phenotype. Nine weeks after induction of EC, obese and lean mice were randomized to receive tirzepatide for 4 weeks. Body and tumor weights, tumor transcriptomic and metabolomic profiles, and serum metabolic markers and chemokines were assessed. RESULTS: Both obese and lean mice began to lose body weight after 2 weeks of tirzepatide treatment, ultimately achieving a significant weight loss of 20.1 % in obese mice and 16.8 % in lean mice. Tirzepatide improved obesity-induced serum adiponectin, leptin, GIP, and C-reactive protein levels. Furthermore, tirzepatide relative to vehicle, effectively reduced tumor growth in obese and lean mice, inhibited the ErbB signaling and glycolysis/gluconeogenesis in tumors of obese mice, and increased O-linked glycosylation biosynthesis and phospholipase D signaling in tumors of lean mice. CONCLUSION: Tirzepatide decreased both mouse weight and tumor growth via effects on metabolic and immune pathways in the EC tumors that differed between obese and lean mice. This novel weight loss treatment deserves further evaluation as an innovative strategy in the management of EC.

Verbatim abstract via PubMed 39388742 ↗

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