Enhanced glucose-induced intracellular signaling promotes insulin hypersecretion: pancreatic beta-cell functional adaptations in a model of genetic obesity and prediabetes

Irles, Esperanza; Ñeco, Patricia; Lluesma, Mónica; Villar-Pazos, Sabrina; Santos-Silva, Junia Carolina; Vettorazzi, Jean F.; Alonso-Magdalena, Paloma; Carneiro, Everardo M.; Boschero, Antonio C.; Nadal, Ángel; Quesada, Ivan

Please use this identifier to cite or link to this item: http://repositorio.unicamp.br/jspui/handle/REPOSIP/202080

Type:	Artigo
Title:	Enhanced glucose-induced intracellular signaling promotes insulin hypersecretion: pancreatic beta-cell functional adaptations in a model of genetic obesity and prediabetes
Author:	Irles, Esperanza Ñeco, Patricia Lluesma, Mónica Villar-Pazos, Sabrina Santos-Silva, Junia Carolina Vettorazzi, Jean F. Alonso-Magdalena, Paloma Carneiro, Everardo M. Boschero, Antonio C. Nadal, Ángel Quesada, Ivan
Abstract:	Obesity is associated with insulin resistance and is known to be a risk factor for type-2 diabetes. In obese individuals, pancreatic beta-cells try to compensate for the increased insulin demand in order to maintain euglycemia. Most studies have reported that this adaptation is due to morphological changes. However, the involvement of beta-cell functional adaptations in this process needs to be clarified. For this purpose, we evaluated different key steps in the glucose-stimulated insulin secretion (GSIS) in intact islets from female ob/ob obese mice and lean controls. Obese mice showed increased body weight, insulin resistance, hyperinsulinemia, glucose intolerance and fed hyperglycemia. Islets from ob/ob mice exhibited increased glucose-induced mitochondrial activity, reflected by enhanced NAD(P)H production and mitochondrial membrane potential hyperpolarization. Perforated patch-clamp examination of beta-cells within intact islets revealed several alterations in the electrical activity such as increased firing frequency and higher sensitivity to low glucose concentrations. A higher intracellular Ca(2+) mobilization in response to glucose was also found in ob/ob islets. Additionally, they displayed a change in the oscillatory pattern and Ca(2+) signals at low glucose levels. Capacitance experiments in intact islets revealed increased exocytosis in individual ob/ob beta-cells. All these up-regulated processes led to increased GSIS. In contrast, we found a lack of beta-cell Ca(2+) signal coupling, which could be a manifestation of early defects that lead to beta-cell malfunction in the progression to diabetes. These findings indicate that beta-cell functional adaptations are an important process in the compensatory response to obesity. Obesity is associated with insulin resistance and is known to be a risk factor for type-2 diabetes. In obese individuals, pancreatic beta-cells try to compensate for the increased insulin demand in order to maintain euglycemia. Most studies have reported
Subject:	Células secretoras de insulina Diabetes Mellitus Obesidade Sinalização do cálcio Insulina - Secreção
Country:	Irlanda
Editor:	Elsevier
Citation:	Molecular And Cellular Endocrinology. v. 404, p. 46-55, 2015-Mar.
Rights:	fechado fechado
Identifier DOI:	10.1016/j.mce.2015.01.033
Address:	https://www.sciencedirect.com/science/article/pii/S0303720715000441
Date Issue:	2015
Appears in Collections:	IB - Artigos e Outros Documentos

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