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Involvement of microsomal prostaglandin E synthase-1 (mPGES-1) in diet-induced adiposity

Published online by Cambridge University Press:  05 October 2018

Pierre Clément
Affiliation:
Aix Marseille Université. Laboratoire de Neurosciences Cognitives, UMR CNRS 7291, France Biomeostasis CRO, La Penne/Huveaune, France
Airault Coraline
Affiliation:
Aix Marseille Université. Laboratoire de Neurosciences Cognitives, UMR CNRS 7291, France
Baril Nathalie
Affiliation:
Fédération de Recherche 3C (FR 3512), Campus St Charles, Marseille, France
Rim Barbouche
Affiliation:
Aix Marseille Université. Laboratoire de Neurosciences Cognitives, UMR CNRS 7291, France
Guillebaud Florent
Affiliation:
Aix Marseille Université. Laboratoire de Neurosciences Cognitives, UMR CNRS 7291, France
Rami Stéphanie
Affiliation:
Aix Marseille Université. Laboratoire de Neurosciences Cognitives, UMR CNRS 7291, France
Save Etienne
Affiliation:
Aix Marseille Université. Laboratoire de Neurosciences Cognitives, UMR CNRS 7291, France
Dallaporta Michel
Affiliation:
Aix Marseille Université. Laboratoire de Neurosciences Cognitives, UMR CNRS 7291, France
Bariohay Bruno
Affiliation:
Biomeostasis CRO, La Penne/Huveaune, France
Troadec Jean Denis
Affiliation:
Aix Marseille Université. Laboratoire de Neurosciences Cognitives, UMR CNRS 7291, France
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Abstract

Type
Abstract
Copyright
Copyright © The Authors 2018 

Low grade inflammation is known to be linked to obesity, and to occur in the early stages of the disease(Reference Thaler, Yi and Schur1). This mechanism is complex and involves numerous organs, cells, and cytokines. In this context, inflammation of white adipose tissue seems to play a key role in the development of obesity(Reference Strissel, Stancheva and Miyoshi2). Because of its properties, prostaglandin E2 (PGE2), an emblematic inflammatory mediator, has been proposed as an actor linking inflammation and obesity. Indeed, PGE2 is involved in mechanisms that are dysregulated in obesity such as lipolysis(Reference Richelsen and Pedersen3) and adipogenesis(Reference Xu, Fu and Miao4). Microsomal prostaglandin E synthase-1 (mPGES-1) is an enzyme which specifically catalyzes the final step of PGE2 biosynthesis.

Interestingly, mPGES-1 invalidation dramatically alters the production of PGE2 during inflammation(Reference Pecchi, Dallaporta and Jean5). In the present work, we sought to determine whether mPGES-1 could contribute to inflammation associated with obesity. First, mRNA expression of mPGES-1 was analyzed using Real-Time PCR, in epididymal white adipose tissue (EAT) of C57BL/6 mice fed with either a normal chow (NC), or a high-fat diet (HFD) during 10 weeks. In a second step, mPGES-1 −/− (KO) mice and wild-type (WT) mice, obtained from heterozygote mating, were also fed with a NC, or a HFD. Body weight and food intake were measured twice a week, and total adiposity was assessed by magnetic resonance imaging (MRI) one week before the end of the HFD period. Then, animals were sacrificed and EAT was collected for RT-PCR analysis. All results are represented as mean ± SEM.

We observed that C57BL/6 mice fed with a HFD during 10 weeks exhibited a significant increase in body weight gain, and a decrease in mRNA expression of mPGES-1 in EAT (table 1). On the other hand, KO mice did not exhibited significant changes in body weight gain after high fat feeding, when compared with their respective control i.e. WT-HFD (table 2). Consistently, MRI acquisition showed that WT-HFD mice exhibited an important increase in total adiposity, but this increase was partially blunted in KO-HFD mice. This phenotype was not explained by a simple reduction in cumulative caloric intake. Interestingly, the increased inflammatory markers mRNA expression (CD68, CCL2) observed in EAT of WT-HFD mice, was reduced in KO-HFD mice. Experiments are under investigations to further characterize mechanisms contributing to the resistance of mPGES-1 KO mice to diet-induced obesity. Altogether, these results suggest that inhibition of mPGES-1 may prevent diet-induced obesity in mice.

Table 1. mRNA expression of mPGES-1 in EAT of diet-induced obese mice.

Student's t-test was used for comparison between groups. Statistical symbol (aC57BL/6-HFD) show diffcrcnccs at P < 0·05.

Table 2. Impact of mPGES-1 invalidation on diet-induced adiposity.

One-way ANOVA was used for comparison groups, and Fisher's test for post-hoc analysis. Statistical symbols (aWT-NC, bKO-NC, cWT-HFD) show differences at P < 0·05.

References

1.Thaler, JP, Yi, CX, Schur, EA, et al. (2012) J Clin Invest 122, 153162.Google Scholar
2.Strissel, KJ, Stancheva, Z, Miyoshi, H et al. (2007) Diabetes 56, 29102918.Google Scholar
3.Richelsen, B & Pedersen, SB (1987) Endocrinology 121, 12211226.Google Scholar
4.Xu, H, Fu, J-L, Miao, Y-F et al. (2016) J Mol Cell Biol 8, 518529.Google Scholar
5.Pecchi, E, Dallaporta, M, Jean, A et al. (2009) Physiol Behav 97, 279–92.Google Scholar
Figure 0

Table 1. mRNA expression of mPGES-1 in EAT of diet-induced obese mice.

Figure 1

Table 2. Impact of mPGES-1 invalidation on diet-induced adiposity.