Adapting the GLP-1-Signaling System to the Treatment of Type 2 Diabetes

Teresa Salvatore; Ornella Carbonara; Domenico Cozzolino; Roberto Torella; Ferdinando Carlo Sasso

doi:10.2174/157339907779802076

ISSN: 1573-3998
E-ISSN: 1875-6417

Adapting the GLP-1-Signaling System to the Treatment of Type 2 Diabetes
Authors: Teresa Salvatore¹, Ornella Carbonara², Domenico Cozzolino³, Roberto Torella⁴ and Ferdinando Carlo Sasso⁵
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¹ Via D. De Dominicis, 8, I-80128 Napoli, Italy. ² Via D. De Dominicis, 8, I-80128 Napoli, Italy. ³ Via D. De Dominicis, 8, I-80128 Napoli, Italy. ⁴ Via D. De Dominicis, 8, I-80128 Napoli, Italy. ⁵ Via D. De Dominicis, 8, I-80128 Napoli, Italy.
Source: Current Diabetes Reviews, Volume 3, Issue 1, Feb 2007, p. 15 - 23
DOI: https://doi.org/10.2174/157339907779802076
- Available online: 01 Feb 2007

Abstract

Glucagon-like peptide-1 (GLP-1) may contribute to the decreased incretin effect characterizing type 2 diabetes. Multiple actions other than insulin secretion stimulation give to GLP-1 a highly desirable profile for an antidiabetic agent. To overcome the need for continuous infusion of the native compound, which is rapidly degraded by dimetyl peptidil peptidase-IV (DPP-IV), analogues with low affinity for this protease have been developed. A second major strategy is represented by DPP-IV inhibitors that act to increase endogenous GLP-1. On the basis of the promising results in clinical trials, the incretin-based therapy may offer an useful option for diabetes management.

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2007-02-01

2025-09-04

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Article Type: Research Article

Keyword(s): DPP-IV inhibitors; GLP-1R agonists; Glucagon-like peptide-1; Incretin effect; Type 2 diabetes

Adapting the GLP-1-Signaling System to the Treatment of Type 2 Diabetes

Abstract

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