Recent Advances in Incretin-Based Pharmacotherapies for the Treatment of Obesity and Diabetes

Mar 18, 2022Frontiers in endocrinology

New Developments in Incretin Medicines for Treating Obesity and Diabetes

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Abstract

has evolved from a hormone with a half-life of ~2-3 min to various formulations including once-weekly drugs.

  • GLP-1 is recognized as a therapeutic target for obesity and type 2 diabetes.
  • has received limited attention due to mixed evidence on its metabolic effects.
  • Recent clinical successes of dual-agonists targeting both GIP and GLP-1 receptors have shown significantly improved body weight and glucose control.
  • The pharmacological profiles of incretin hormones are being continuously refined to enhance their therapeutic potential.

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Key numbers

50 to 70%
Weight Loss Achievement
Percentage of patients achieving >5% weight reduction with liraglutide.
47 to 57%
Weight Loss with Tirzepatide
Patients losing >10% body weight after 40 weeks of tirzepatide treatment.

Full Text

What this is

  • The review discusses advances in incretin-based pharmacotherapies targeting and for obesity and diabetes treatment.
  • It highlights the evolution of GLP-1R agonists from native hormones to long-acting formulations.
  • The review also addresses the emerging interest in GIPR agonism and the development of dual-agonist therapies.

Essence

  • Incretin-based therapies, particularly GLP-1R agonists, have evolved significantly, demonstrating efficacy in weight loss and glycemic control. Recent dual-agonist approaches targeting both and receptors show promise for enhanced metabolic outcomes.

Key takeaways

  • GLP-1R agonists like semaglutide and liraglutide have shown effective weight loss, with up to 70% of patients achieving >5% weight reduction. These agents also improve cardiovascular health in patients with type 2 diabetes.
  • Tirzepatide, a dual-agonist for and , demonstrated superior weight loss and glycemic control compared to semaglutide in clinical trials, with 47–57% of patients losing >10% body weight.

Caveats

  • The review notes that clinical trials for tirzepatide had lower enrollment of racial and ethnic minorities, raising concerns about the generalizability of the findings.
  • While GLP-1R agonists improve outcomes, individual responses vary significantly, necessitating precision medicine approaches for optimal treatment.

Definitions

  • GLP-1: Glucagon-like peptide-1, an incretin hormone that enhances insulin secretion and reduces appetite.
  • GIP: Glucose-dependent insulinotropic polypeptide, an incretin hormone that stimulates insulin secretion in response to food intake.

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