The PPAR<i>α</i>/<i>γ</i> dual agonist chiglitazar improves insulin resistance and dyslipidemia in MSG obese rats

Li, Pingping; Song, Shan; Chen, Yue-Teng; Ning, Zhiqiang; Sun, Sujuan; Liu, Quan; Lu, Xianping; Xie, Min; Shen, Zhufang

doi:10.1038/sj.bjp.0706745

Cited by 56 publications

(44 citation statements)

References 35 publications

(40 reference statements)

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“…Chiglitazar (33), a PPAR / agonist, by suppressing the expression of genes for the key gluconeogenic enzymes PEPCK and G-6-Pase and upregulating mRNA expression of genes involved in NEFA oxidation, demonstrated to reduce insulin resistance and to improve glucose tolerance and lipid profiles in monosodium L-glutamate obese rats [273]. Unfortunately, this study does not report data on liver fibrosis.…”

Section: Dual or Pan Ppars Agonistsmentioning

confidence: 58%

Hepatic PPARs: Their Role in Liver Physiology, Fibrosis and Treatment

Zardi¹,

Navarini²,

Sambataro³

et al. 2013

CMC

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Abstr act: Complex molecular and cellular mechanisms are involved in the pathway of liver fibrosis. Activation and transformation of hepatic stellate cells (HSCs) are considered the two main reasons for the cause and development of liver fibrosis. The peroxisome proliferator-activated receptors (PPARs) belonging to the family of ligand-activated transcription factors play a key role in liver homeostasis, regulating adipogenesis and inhibiting fibrogenesis in HSCs. Normal transcriptional function of PPARs contributes to maintain HSCs in quiescent phase. A reduced expression of PPARs in HSCs greatly induces a progression of liver fibrosis and an increased production of collagen. Here, we discuss role and function of PPARs and we take into consideration molecular factors able to reduce PPARs activity in HSCs. Finally, although further validations are needed, we illustrate novel strategies available from in vitro and animal studies on how some PPARs-agonists have been proved effective as antifibrotic substances in liver disease.

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Section: Dual or Pan Ppars Agonistsmentioning

confidence: 58%

Hepatic PPARs: Their Role in Liver Physiology, Fibrosis and Treatment

Zardi¹,

Navarini²,

Sambataro³

et al. 2013

CMC

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“…Studies have shown that successful beta cell adaptation to insulin resistance includes increasing beta cell mass via hypertrophy and/or hyperplasia [30]. However, few studies have been conducted to evaluate the endocrine characteristics of the pancreas in MSG-treated obese rats, and the data that have been reported are contradictory [22,31]. The proliferation of pancreatic islets is modulated by parasympathetic vagal activity [32].…”

Section: Discussionmentioning

confidence: 99%

Glycolytic and Mitochondrial Metabolism in Pancreatic Islets from MSG-Treated Obese Rats Subjected to Swimming Training

Leite

Ferreira

Rickli

et al. 2013

Cell Physiol Biochem

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Backgrounds/Aims: Obese rats obtained by neonatal monosodium glutamate (MSG) administration present insulin hypersecretion. The metabolic mechanism by which glucose catabolism is coupled to insulin secretion in the pancreatic β-cells from MSG-treated rats is understood. The purpose of this study was to evaluate glucose metabolism in pancreatic islets from MSG-treated rats subjected to swimming training. Methods: MSG-treated and control (CON) rats swam for 30 minutes (3 times/week) over a period of 10 weeks. Pancreatic islets were isolated and incubated with glucose in the presence of glycolytic or mitochondrial inhibitors. Results: Swimming training attenuated fat pad accumulation, avoiding changes in the plasma levels of lipids, glucose and insulin in MSG-treated rats. Adipocyte and islet hypertrophy observed in MSG-treated rats were attenuated by exercise. Pancreatic islets from MSG-treated obese rats also showed insulin hypersecretion, greater glucose transporter 2 (GLUT2) expression, increased glycolytic flux and reduced mitochondrial complex III activity. Conclusion: Swimming training attenuated islet hypertrophy and normalised GLUT2 expression, contributing to a reduction in the glucose responsiveness of pancreatic islets from MSG-treated rats without altering glycolytic flux. However, physical training increased the activity of mitochondrial complex III in pancreatic islets from MSG-treated rats without a subsequent increase in glucose-induced insulin secretion.

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“…This could perhaps be indicative of onset of hepatic insulin resistance, as reported in a previous study (35), which has yet to affect whole body insulin resistance or glucose tolerance. Although the use of HOMA as a measurement of insulin resistance in rodent studies is quite common (14,27), it is also controversial (38) and better suited to larger cohorts. Nevertheless, our finding of elevated HOMA in the Restricted female rats suggests that alterations in insulin sensitivity could be occurring in our model of restriction that might be more readily detected by more sensitive measures such as a euglycemic hyperinsulinemic clamp.…”

Section: Discussionmentioning

confidence: 99%