The dual glucose-dependent insulinotropic polypeptide (GIP) and glucagon-like peptide-1 (GLP-1) receptor agonist tirzepatide: a novel cardiometabolic therapeutic prospect

Nov 25, 2021Cardiovascular diabetology

Tirzepatide, a new medicine that activates two blood sugar hormones, as a potential heart and metabolism treatment

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Abstract

Tirzepatide, a dual GIP and GLP-1 receptor agonist, significantly lowers glucose levels and improves insulin sensitivity.

  • , including GLP-1 and GIP, play key roles in insulin secretion and glucose regulation.
  • The insulin response to GIP is significantly reduced in type 2 diabetes mellitus (T2DM), leading to its previous dismissal as a therapeutic target.
  • Recent findings suggest that resistance to GIP can be reversed with improved glycemic control.
  • Tirzepatide is administered as a weekly subcutaneous injection and shows potential in reducing weight and positively modifying lipid profiles.
  • The development of tirzepatide and other dual agonists may represent a significant advancement in managing cardiometabolic conditions.
  • Further research is needed to assess the long-term effects and cardiovascular benefits of these treatments.

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Key numbers

30%
Increase in normoglycemia
Achieved < 5.7% in a phase 2b trial.
2.4%
reduction
Reduction in the 15 mg dose group compared to dulaglutide 1.5 mg.
25%
Weight loss
Lost ≄ 15% of body weight in a 26-week phase 2b trial.

Key figures

Fig. 1
Main combined effects of dual and receptor agonist on physiological functions
Highlights the broad physiological impact of dual GIP and GLP-1 agonists on metabolic and pancreatic functions
12933_2021_1412_Fig1_HTML
  • Panel single diagram
    Shows dual agonist effects from duodenojejunal K cells (GIP) and ileocolonic L cells (GLP-1) increasing , insulin sensitivity, insulin secretion, triglyceride clearance, satiety, , , and ventricular contractility
  • Panel single diagram
    Shows dual agonist effects decreasing glucagon secretion, gastric secretion, gastric emptying, appetite, , hepatic glucose production, gastrointestinal motility, and

Full Text

What this is

  • This review discusses the dual receptor agonist tirzepatide, targeting GIP and GLP-1, as a novel treatment for type 2 diabetes mellitus (T2DM).
  • Tirzepatide shows promise in lowering glucose levels, improving insulin sensitivity, and aiding weight loss.
  • The review emphasizes the potential of tirzepatide in managing cardiometabolic diseases, though long-term effects remain to be evaluated.

Essence

  • Tirzepatide, a dual GIP and GLP-1 receptor agonist, effectively lowers glucose levels and promotes weight loss in T2DM patients, presenting a new therapeutic avenue for cardiometabolic management.

Key takeaways

  • Tirzepatide has shown significant efficacy in glucose control and weight reduction in T2DM patients. In a phase 2b trial, 30% of patients on a 15 mg dose achieved normoglycemia with < 5.7%, and 25% lost ≄ 15% of their body weight.
  • Tirzepatide outperformed dulaglutide in reducing levels, achieving reductions of 1.6%, 2.0%, and 2.4% in the 5, 10, and 15 mg dose groups, respectively, compared to 1.1% for dulaglutide.
  • In the SURPASS-2 trial, all tirzepatide doses led to greater reductions in and weight compared to semaglutide, indicating its superior efficacy in T2DM management.

Caveats

  • Long-term effects of tirzepatide are still unknown, necessitating further studies to confirm cardiovascular benefits and safety.
  • The review does not provide extensive data on potential adverse effects beyond gastrointestinal issues, which may limit understanding of the full safety profile.

Definitions

  • Incretin hormones: Peptides released in the intestine that stimulate insulin secretion in response to nutrient presence.
  • HbA1C: A measure of average blood glucose levels over the past 2-3 months, used to diagnose and monitor diabetes.

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