Physiological development of insulin secretion, calcium channels, and GLUT2 expression of pancreatic rat β-cells

Navarro-Tableros, Víctor; Fiordelisio, Tatiana; Hernández‐Cruz, Arturo; Hiriart, Marcia

doi:10.1152/ajpendo.00457.2006

Cited by 58 publications

(67 citation statements)

References 53 publications

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“…We further document that, during development, the levels of Cx36 expression correlate with those of the insulin gene, as recently reported in humans [29]. Beta cells of neonatal islets express significantly less insulin mRNA than those of adult rats [8], a difference that cannot be explained merely by developmental changes in beta cell number/volume [3]. Our data indicate that increased CX36 signalling may be required to achieve proper insulin expression, an essential landmark of beta cell maturation, a consideration which, in turn, raises the intriguing possibility that the CX36 and beta cell maturation events may not only be coincidental but Fig.…”

Section: Discussionsupporting

confidence: 85%

“…M, molecular weight markers; F, fetus; N, neonatal; Y, young; A, adult. *p<0.05 vs neonatal and fetal values depolarisation and Ca +2 handling [1,2,4,7,8,24], it is conceivable that their modest expression of Cx36, gap junctions and beta cell coupling could account for their poor glucose-induced insulin secretion. Consistent with this view, we now show that a postnatal increase in the levels of the CX36 protein, the abundance of gap junctions and the extent of beta cell coupling accompanies the in vivo acquisition of glucose responsiveness, as previously suggested by preliminary in vitro experiments [9].…”

Section: Discussionmentioning

confidence: 99%

“…It has long been known that this glucose responsiveness is normally established in the few days that follow birth, even though beta cells are already equipped in the late prenatal period with most of their adult features [3][4][5][6][7][8]. Several events occurring during the early neonatal period, including changes in K + membrane permeability, production of GLUT2, protein kinase C-alpha, Ca 2+ channels and key enzymes of the NADH shuttles, are implicated in the maturation of beta cell function [1,2,[4][5][6][7][8][23][24][25]. We now show that gap junction/CX36 signalling, which contributes significantly to the proper function of adult beta cells [17, Fig.…”

Section: Discussionmentioning

confidence: 99%

“…When compared with adult islets, fetal and neonatal islets from different species exhibit a reduced secretory response to glucose and other secretagogues [1][2][3][4][5][6][7][8]. The nature of this poor responsiveness is not fully understood, and has been variably attributed to many factors, including fuel metabolites, intracellular signals, hormones and other environmental conditions [1][2][3][8][9][10][11].…”

Section: Introductionmentioning

confidence: 99%

“…The nature of this poor responsiveness is not fully understood, and has been variably attributed to many factors, including fuel metabolites, intracellular signals, hormones and other environmental conditions [1][2][3][8][9][10][11].…”

Section: Introductionmentioning

confidence: 99%

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Beta cell coupling and connexin expression change during the functional maturation of rat pancreatic islets

et al. 2010

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Aims/hypothesis Cell-cell coupling mediated by gap junctions formed from connexin (CX) contributes to the control of insulin secretion in the endocrine pancreas. We investigated the cellular production and localisation of CX36 and CX43, and gap junction-mediated beta cell coupling in pancreatic islets from rats of different ages, displaying different degrees of maturation of insulin secretion. Methods The presence and distribution of islet connexins were assessed by immunoblotting and immunofluorescence. The expression of connexin genes was evaluated by RT-PCR and quantitative real-time PCR. The ultrastructure of gap junctions and the function of connexin channels were assessed by freeze-fracture electron microscopy and tracer microinjection, respectively. Results Young and adult beta cells, which respond to glucose, expressed significantly higher levels of Cx36 (also known as Gjd2) than fetal and newborn beta cells, which respond poorly to the sugar. Accordingly, adult beta cells also showed a significantly higher membrane density of gap junctions and greater intercellular exchange of ethidium bromide than newborn beta cells. Cx43 (also known as Gja1) was not expressed by beta cells, but was located in various cell types at the periphery of fetal and newborn islets. Conclusions/interpretation These findings show that the pattern of connexins, gap junction membrane density and coupling changes in islets during the functional maturation of beta cells.

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Section: Discussionsupporting

confidence: 85%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Beta cell coupling and connexin expression change during the functional maturation of rat pancreatic islets

et al. 2010

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Cardiotoxin‐I: An Unexpectedly Potent Insulinotropic Agent

et al. 2012

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Insulin secretion from pancreatic β-cells is a complex process, involving the integration and interaction of multiple external and internal stimuli, in which glucose plays a major role. Understanding the physiology leading to insulin release is a crucial step toward the identification of new targets. In this study, we evaluated the presence of insulinotropic metabolites in Naja kaouthia snake venom. Only one fraction, identified as cardiotoxin-I (CTX-I) was able to induce insulin secretion from INS-1E cells without affecting cell viability and integrity, as assessed by MTT and LDH assays. Interestingly, CTX-I was also able to stimulate insulin secretion from INS-1E cells even in the absence of glucose. Although cardiotoxins have been characterized as potent hemolytic agents and vasoconstrictors, CTX-I was unable to induce direct hemolysis of human erythrocytes or to induce potent vasoconstriction. As such, this newly identified insulin-releasing toxin will surely enrich the pool of existing tools to study β-cell physiology or even open a new therapeutic avenue.

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High Fat Programming of β-Cell Failure

Cerf

2010

Advances in Experimental Medicine and Biology

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High saturated fat intake contributes to insulin resistance, beta-cell failure, and type 2 diabetes. Developmental programming refers to a stimulus or insult during critical periods of life which includes fetal and subsequent early neonatal life. Programming alters offspring physiology and metabolism with both immediate and lasting consequences. Maternal nutrition in gestation and lactation shapes offspring development and health. A high saturated fat diet ingested by mothers during gestation and/or lactation is a form of nutritional insult that induces diabetogenic changes in offspring physiology and metabolism. High fat programming is induced by maternal high saturated fat intake during defined periods of gestation and/or lactation and programs the physiology and metabolism of the offspring in early life. This more recently adopted form of developmental programming reflects society in both affluent and developing countries. High fat programming induces adverse changes in beta-cell development and function in neonatal and weanling offspring. These changes are characterized by compromised beta-cell development and function, evident by altered expression of key factors that maintain the beta-cell phenotype. High fat programming is likely to result in beta-cell failure and eventual type 2 diabetes.

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Physiological development of insulin secretion, calcium channels, and GLUT2 expression of pancreatic rat β-cells

Cited by 58 publications

References 53 publications

Beta cell coupling and connexin expression change during the functional maturation of rat pancreatic islets

Beta cell coupling and connexin expression change during the functional maturation of rat pancreatic islets

Cardiotoxin‐I: An Unexpectedly Potent Insulinotropic Agent

High Fat Programming of β-Cell Failure

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