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Roles of <scp>glucose‐dependent</scp> insulinotropic polypeptide in <scp>diet‐induced</scp> obesity

Yusuke Seino, Y. Yamazaki

2022Journal of Diabetes Investigation18 citationsDOIOpen Access PDF

Abstract

Glucose-dependent insulinotropic polypeptide (GIP) and glucagon-like peptide-1 (GLP-1) are incretins that play an important role in glucose metabolism, by increasing glucose-induced insulin secretion from pancreatic β-cells and help regulate bodyweight. Although they show a similar action on glucose-induced insulin secretion, two incretins are distinct in various aspects. GIP is secreted from enteroendocrine K cell mainly expressed in the upper small intestine, and GLP-1 is secreted from enteroendocrine L cells mainly expressed in the lower small intestine and colon by the stimulation of various nutrients. The mechanism of GIP secretion induced by nutrients, especially carbohydrates, is different from that of GLP-1 secretion. GIP promotes fat deposition in adipose tissue, and contributes to fat-induced obesity. In contrast, GLP-1 participates in reducing bodyweight by suppressing food consumption and/or slowing gastric emptying. There is substantial evidence that GIP and GLP-1 might differently contribute to bodyweight control. Although meal contents influence both glycemic and weight control, we do not fully understand whether incretin actions differ depending on the contents of the meal and what kind of signaling is involved in its context. We focus on the molecular mechanism of GIP secretion induced by nutrients, as well as the roles of GIP in weight changes caused by various diets.

Topics & Concepts

IncretinEndocrinologyGastric inhibitory polypeptideInternal medicineEnteroendocrine cellGlucagon-like peptide-1InsulinSecretionAdipose tissueMedicineType 2 diabetesDiabetes mellitusGlucagonEndocrine systemHormoneDiabetes Treatment and ManagementBiochemical Analysis and Sensing TechniquesRegulation of Appetite and Obesity
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