Palmitate-induced beta-cell dysfunction is associated with excessive NO pro-duction and is reversed by thiazolidinedione-mediated inhibition of GPR40 transduction mechanisms
Meidute, Sandra LU ; Lundquist, Ingmar LU ; Galvanovskis, Juris ; Flodgren, Erik LU ; Olde, Björn LU and Salehi, S Albert LU
(2008)
In PLoS ONE
- Abstract
- Background: Type 2 diabetes often displays hyperlipidemia. We examined palmitate effects on pancreatic islet function in relation to FFA receptor GPR40, NO generation, insulin release, and the PPARgama agonistic thiazolidinedione, rosiglitazone. Principal findings: Rosiglitazone suppressed acute palmitate-stimulated GPR40-transduced PI hydrolysis in HEK293 cells and insulin release from MIN6c cells and mouse islets. Culturing islets 24 h with palmitate at 5 mmol/l glucose induced beta-cell iNOS expression as revealed by confocal microscopy and in-creased the activities of ncNOS and iNOS associated with suppression of glucose-stimulated insulin response. Rosiglitazone reversed these effects. The expression of iNOS after high-glucose... (More)
- Background: Type 2 diabetes often displays hyperlipidemia. We examined palmitate effects on pancreatic islet function in relation to FFA receptor GPR40, NO generation, insulin release, and the PPARgama agonistic thiazolidinedione, rosiglitazone. Principal findings: Rosiglitazone suppressed acute palmitate-stimulated GPR40-transduced PI hydrolysis in HEK293 cells and insulin release from MIN6c cells and mouse islets. Culturing islets 24 h with palmitate at 5 mmol/l glucose induced beta-cell iNOS expression as revealed by confocal microscopy and in-creased the activities of ncNOS and iNOS associated with suppression of glucose-stimulated insulin response. Rosiglitazone reversed these effects. The expression of iNOS after high-glucose culturing was unaffected by rosiglitazone. Downregulation of GPR40 by antisense treatment abrogated GPR40 expression and suppressed palmitate-induced iNOS activity and insulin release. Conclusion: We conclude that, in addition to mediating acute FFA-stimulated insulin release, GPR40 is an important regulator of iNOS expression and dysfunctional insulin release during long-term exposure to FFA. The adverse effects of palmitate were counteracted by rosiglitazone at GPR40, suggesting that thiazolidinediones are beneficial for beta-cell function in hyperlipidemic type 2 diabetes. (Less)
Please use this url to cite or link to this publication:
https://lup.lub.lu.se/record/1157362
- author
- Meidute, Sandra
LU
; Lundquist, Ingmar
LU
; Galvanovskis, Juris
; Flodgren, Erik
LU
; Olde, Björn
LU
and Salehi, S Albert
LU
- organization
- publishing date
- 2008
- type
- Contribution to specialist publication or newspaper
- publication status
- published
- subject
- keywords
- inducible nitric oxide synthase (iNOS), neural constitutive nitric ox-ide synthase (ncNOS), GPR40, palmitate, glucose-stimulated insulin release
- categories
- Popular Science
- in
- PLoS ONE
- publisher
- Public Library of Science (PLoS)
- language
- English
- LU publication?
- yes
- id
- 3783f14d-22a2-46c8-906f-a8f6d914868e (old id 1157362)
- alternative location
- http://www.plosone.org/article/info%3Adoi%2F10.1371%2Fjournal.pone.0002182
- http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2366067/
- http://www.ncbi.nlm.nih.gov/pubmed/18478115
- date added to LUP
- 2016-04-04 14:18:57
- date last changed
- 2023-04-18 18:02:40
@misc{3783f14d-22a2-46c8-906f-a8f6d914868e,
abstract = {{Background: Type 2 diabetes often displays hyperlipidemia. We examined palmitate effects on pancreatic islet function in relation to FFA receptor GPR40, NO generation, insulin release, and the PPARgama agonistic thiazolidinedione, rosiglitazone. Principal findings: Rosiglitazone suppressed acute palmitate-stimulated GPR40-transduced PI hydrolysis in HEK293 cells and insulin release from MIN6c cells and mouse islets. Culturing islets 24 h with palmitate at 5 mmol/l glucose induced beta-cell iNOS expression as revealed by confocal microscopy and in-creased the activities of ncNOS and iNOS associated with suppression of glucose-stimulated insulin response. Rosiglitazone reversed these effects. The expression of iNOS after high-glucose culturing was unaffected by rosiglitazone. Downregulation of GPR40 by antisense treatment abrogated GPR40 expression and suppressed palmitate-induced iNOS activity and insulin release. Conclusion: We conclude that, in addition to mediating acute FFA-stimulated insulin release, GPR40 is an important regulator of iNOS expression and dysfunctional insulin release during long-term exposure to FFA. The adverse effects of palmitate were counteracted by rosiglitazone at GPR40, suggesting that thiazolidinediones are beneficial for beta-cell function in hyperlipidemic type 2 diabetes.}},
author = {{Meidute, Sandra and Lundquist, Ingmar and Galvanovskis, Juris and Flodgren, Erik and Olde, Björn and Salehi, S Albert}},
keywords = {{inducible nitric oxide synthase (iNOS); neural constitutive nitric ox-ide synthase (ncNOS); GPR40; palmitate; glucose-stimulated insulin release}},
language = {{eng}},
publisher = {{Public Library of Science (PLoS)}},
series = {{PLoS ONE}},
title = {{Palmitate-induced beta-cell dysfunction is associated with excessive NO pro-duction and is reversed by thiazolidinedione-mediated inhibition of GPR40 transduction mechanisms}},
url = {{http://www.plosone.org/article/info%3Adoi%2F10.1371%2Fjournal.pone.0002182}},
year = {{2008}},
}