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. 2019 May;121(10):1097-1107.
doi: 10.1017/S0007114519000461. Epub 2019 Mar 5.

Dietary α-lactalbumin alters energy balance, gut microbiota composition and intestinal nutrient transporter expression in high-fat diet-fed mice

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Dietary α-lactalbumin alters energy balance, gut microbiota composition and intestinal nutrient transporter expression in high-fat diet-fed mice

Serena Boscaini et al. Br J Nutr. 2019 May.

Abstract

Recently there has been a considerable rise in the frequency of metabolic diseases, such as obesity, due to changes in lifestyle and resultant imbalances between energy intake and expenditure. Whey proteins are considered as potentially important components of a dietary solution to the obesity problem. However, the roles of individual whey proteins in energy balance remain poorly understood. This study investigated the effects of a high-fat diet (HFD) containing α-lactalbumin (LAB), a specific whey protein, or the non-whey protein casein (CAS), on energy balance, nutrient transporters expression and enteric microbial populations. C57BL/6J mice (n 8) were given an HFD containing either 20 % CAS or LAB as protein sources or a low-fat diet containing CAS for 10 weeks. HFD-LAB-fed mice showed a significant increase in cumulative energy intake (P=0·043), without differences in body weight, energy expenditure, locomotor activity, RER or subcutaneous and epididymal white adipose tissue weight. HFD-LAB intake led to a decrease in the expression of glut2 in the ileum (P=0·05) and in the fatty acid transporter cd36 (P<0·001) in both ileum and jejunum. This suggests a reduction in absorption efficiency within the small intestine in the HFD-LAB group. DNA from faecal samples was used for 16S rRNA-based assessment of intestinal microbiota populations; the genera Lactobacillus, Parabacteroides and Bifidobacterium were present in significantly higher proportions in the HFD-LAB group. These data indicate a possible functional relationship between gut microbiota, intestinal nutrient transporters and energy balance, with no impact on weight gain.

Keywords: CAS casein; CD36 cluster differentiation 36; FATP4 fatty acid transporter protein 4; HFD high-fat diet; LAB α-lactalbumin; LFD low-fat diet; Lf lactoferrin; WPI whey protein isolate; eWAT epididymal white adipose tissue; fasn fatty acid synthase; npy neuropeptide Y; pomc proopiomelanocortin; sWAT subcutaneous white adipose tissue; Dietary α-lactalbumin; Energy balance; Gut microbiota; High-fat diet; Nutrient transporter expression; Whey proteins.

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