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Diet-induced obesity in ad libitum-fed mice: food texture overrides the effect of macronutrient composition

Published online by Cambridge University Press:  06 August 2012

Charles Desmarchelier*
Affiliation:
Molecular Nutrition Unit, ZIEL – Research Center for Nutrition and Food Sciences, Technische Universität München (TUM), Gregor-Mendel-Strasse 2, 85350 Freising-Weihenstephan, Germany
Tobias Ludwig
Affiliation:
Clinical Nutritional Medicine, ZIEL – Research Center for Nutrition and Food Sciences, Technische Universität München (TUM), Gregor-Mendel-Strasse 2, 85350 Freising-Weihenstephan, Germany
Ronny Scheundel
Affiliation:
Molecular Nutrition Unit, ZIEL – Research Center for Nutrition and Food Sciences, Technische Universität München (TUM), Gregor-Mendel-Strasse 2, 85350 Freising-Weihenstephan, Germany
Nadine Rink
Affiliation:
Molecular Nutritional Medicine (Else Kröner-Fresenius Center), ZIEL – Research Center for Nutrition and Food Sciences, Technische Universität München (TUM), Gregor-Mendel-Strasse 2, 85350 Freising-Weihenstephan, Germany
Bernhard L. Bader
Affiliation:
Clinical Nutritional Medicine, ZIEL – Research Center for Nutrition and Food Sciences, Technische Universität München (TUM), Gregor-Mendel-Strasse 2, 85350 Freising-Weihenstephan, Germany
Martin Klingenspor
Affiliation:
Molecular Nutritional Medicine (Else Kröner-Fresenius Center), ZIEL – Research Center for Nutrition and Food Sciences, Technische Universität München (TUM), Gregor-Mendel-Strasse 2, 85350 Freising-Weihenstephan, Germany
Hannelore Daniel
Affiliation:
Molecular Nutrition Unit, ZIEL – Research Center for Nutrition and Food Sciences, Technische Universität München (TUM), Gregor-Mendel-Strasse 2, 85350 Freising-Weihenstephan, Germany
*
*Corresponding author: C. Desmarchelier, fax +49 81 61 71 39 99, email charles.desmarchelier@univ-amu.fr
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Abstract

Diet-induced obesity in mice can be achieved through the use of diets with different macronutrient compositions and textures. We aimed at determining the contribution of macronutrient composition to obesity development and associated pathophysiological changes in mice. C57BL/6N mice were offered a control, a high-fat or a Western-style diet, either as pellet (H for hard) or with identical composition in powder form (S for soft), resulting in C-S, C-H, HF-H, HF-S, W-H and W-S groups, respectively. Body fat distribution, expression levels of selected target genes in adipose tissues, clinical chemistry and hormone concentration in the blood, as well as liver TAG content were measured. The most striking finding was that all mice fed the different powder diets developed obesity with similar weight gain, whereas among the mice fed the pellet diets, only those given the HF and W diets became obese. This allowed us to separate diet-specific effects from obesity-mediated effects. Irrespective of the food texture, the W diet induced a more severe hepatosteatosis and higher activities of serum transaminases compared with the two other diets. Adipose tissue gene expression analysis revealed that leptin and adiponectin levels were not affected by the dietary composition per se, whereas uncoupling protein 1 and 11β-hydroxysteroid dehydrogenase type 1 levels were decreased by both dietary composition and changes in body weight. In conclusion, diets differing in macronutrient composition elicit specific pathophysiological changes, independently of changes in body weight. A diet high in both fat and sugars seems to be more deleterious for the liver than a HF diet.

Information

Type
Full Papers
Copyright
Copyright © The Authors 2012
Figure 0

Table 1 Composition of the different diets employed*

Figure 1

Fig. 1 Body-weight changes in mice receiving the different diets. (A) Body-weight development in mice receiving the different diets provided as pellets (cohorts 1 and 3). Values are means, with their standard errors represented by vertical bars (C-H (◆): n 20; HF-H (): n 20; W-H (○): n 12). (B) Body-weight development in mice receiving the different powder diets (cohorts 2 and 3). Values are means, with their standard errors represented by vertical bars (C-S (◇): n 20; HF-S (□): n 19; W-S (●): n 12).

Figure 2

Table 2 Final body weight, cumulative food, energy, water and macronutrient intake in mice receiving the different diets either provided in pellet or powder form* (Mean values with their standard errors)

Figure 3

Table 3 Organ weight* (Mean values with their standard errors)

Figure 4

Table 4 Food intake over short periods of time following overnight food deprivation* (Mean values with their standard errors)

Figure 5

Table 5 Serum clinical chemistry and adipokine concentrations (Mean values with their standard errors)

Figure 6

Fig. 2 Liver weight and intrahepatic TAG in mice receiving the different diets. Across all mice and within lines, body weight was significantly correlated with liver weight: r2 0·67, n 66, P< 0·001; C-H (◆): r2 0·00, slope 0·00, n 11, P= 0·955; HF-H (): r2 0·80, slope 0·11, n 10, P< 0·001; W-H (○): r2 0·89, slope 0·15, n 12, P< 0·001; C-S (◇): r2 0·81, slope 0·11, n 11, P< 0·001; HF-S (□): r2 0·80, slope 0·11, n 11, P< 0·001; W-S (●): r2 0·86, slope 0·16, n 11, P< 0·001. a,b,cFor a given group, regression lines with unlike letters indicate a significantly different diet × texture interaction. There were significant body-weight (P< 0·001), diet (P< 0·001) and texture (P< 0·001) effects.

Figure 7

Table 6 Relative expression of the selected target genes in visceral adipose tissues* (Mean values with their standard errors)

Supplementary material: File

Desmarchelier Supplementary Material

Table S1

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