[Postprandial hyperglycemia. II. Pharmacological approaches].

Rev Med Liege

Service de Diabétologie, Nutrition et Maladies métaboliques, Département de Médecine, CHU Sart Tilman.

Published: April 2002

AI Article Synopsis

  • Recent advancements in pharmacology aim to manage postprandial hyperglycaemia through different mechanisms, including slowing carbohydrate absorption and enhancing insulin release after meals.
  • Certain hormones and alpha-glucosidase inhibitors can help in slowing gastric emptying and digestion, assisting in better glucose control.
  • Various drugs like glinides and short-acting insulin analogues are being used for more effective insulin management, while new approaches to inhibit glucagon secretion are also in development.

Article Abstract

Besides dietary approaches, various pharmacological means have been recently developed in order to better control postprandial hyperglycaemia. This objective may be obtained: 1) by slowing down the intestinal absorption of carbohydrates; 2) by insuring a better insulin priming soon after the meal; and 3) by inhibiting post-prandial glucagon secretion or action. Some hormones (amylin, glucagon-like peptide-1) can slow gastric emptying while alpha-glucosidase inhibitors (acarbose, miglitol) retard intestinal digestion and resorption of complex carbohydrates. A more physiological post-meal profile of insulin may be obtained in type 2 diabetes by using new insulin secretagogues of the glinide family (repaglinide, nateglinide) with an earlier and shorter insulinotropic action or, mainly in type 1 diabetes but also in type 2 diabetes, by using short-acting insulin analogues (lispro. Asp B28) or inhated insulin the action of which is faster than that of subcutaneous insulin. Post-prandial glucagon secretion can be inhibited by amylin. GLP-1 or insulin while other glucagon antagonists are currently in development.

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