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Dietary fat drives whole-body insulin resistance and promotes intestinal inflammation independent of body weight gain

Authors :
Jensen, Benjamin Anderschou Holbech
Nielsen, Thomas Svava
Fritzen, Andreas Mæchel
Holm, Jacob Bak
Fjære, Even
Serup, Annette Karen Lundbeck
Borkowski, Kamil
Risis, Steve
Pærregaard, Simone I.
Søgaard, Ida
Poupeau, Audrey Angélique G
Poulsen, Michelle
Ma, Tao
Sina, Christian
Kiens, Bente
Madsen, Lise
Kristiansen, Karsten
Treebak, Jonas Thue
Jensen, Benjamin Anderschou Holbech
Nielsen, Thomas Svava
Fritzen, Andreas Mæchel
Holm, Jacob Bak
Fjære, Even
Serup, Annette Karen Lundbeck
Borkowski, Kamil
Risis, Steve
Pærregaard, Simone I.
Søgaard, Ida
Poupeau, Audrey Angélique G
Poulsen, Michelle
Ma, Tao
Sina, Christian
Kiens, Bente
Madsen, Lise
Kristiansen, Karsten
Treebak, Jonas Thue
Source :
Jensen , B A H , Nielsen , T S , Fritzen , A M , Holm , J B , Fjære , E , Serup , A K L , Borkowski , K , Risis , S , Pærregaard , S I , Søgaard , I , Poupeau , A A G , Poulsen , M , Ma , T , Sina , C , Kiens , B , Madsen , L , Kristiansen , K & Treebak , J T 2016 , ' Dietary fat drives whole-body insulin resistance and promotes intestinal inflammation independent of body weight gain ' , Metabolism , vol. 65 , no. 12 , pp. 1706-1719 .
Publication Year :
2016

Abstract

BACKGROUND: The obesogenic potential of high-fat diets (HFD) in rodents is attenuated when the protein:carbohydrate ratio is increased. However, it is not known if intake of an HFD irrespective of the protein:carbohydrate ratio and in the absence of weight gain, affects glucose homeostasis and the gut microbiota.METHODS: We fed C57BL6/J mice 3 different HFDs with decreasing protein:carbohydrate ratios for 8weeks and compared the results to a LFD reference group. We analyzed the gut microbiota composition by 16S rDNA amplicon sequencing and the intestinal gene expression by real-time PCR. Whole body glucose homeostasis was evaluated by insulin and glucose tolerance tests as well as by a hyperinsulinemic euglycemic clamp experiment.RESULTS: Compared with LFD-fed reference mice, HFD-fed mice, irrespective of protein:carbohydrate ratio, exhibited impaired glucose tolerance, whereas no differences were observed during insulin tolerance tests. The hyperinsulinemic euglycemic clamp revealed tissue-specific effects on glucose homeostasis in all HFD-fed groups. HFD-fed mice exhibited decreased insulin-stimulated glucose uptake in white but not in brown adipose tissue, and sustained endogenous glucose production under insulin-stimulated conditions. We observed no impairment of insulin-stimulated glucose uptake in skeletal muscles of different fiber type composition. HFD-feeding altered the gut microbiota composition paralleled by increased expression of pro-inflammatory cytokines and genes involved in gluconeogenesis in intestinal epithelial cells of the jejunum.CONCLUSIONS: Intake of a HFD profoundly affected glucose homeostasis, gut inflammatory responses, and gut microbiota composition in the absence of fat mass accretion.

Details

Database :
OAIster
Journal :
Jensen , B A H , Nielsen , T S , Fritzen , A M , Holm , J B , Fjære , E , Serup , A K L , Borkowski , K , Risis , S , Pærregaard , S I , Søgaard , I , Poupeau , A A G , Poulsen , M , Ma , T , Sina , C , Kiens , B , Madsen , L , Kristiansen , K & Treebak , J T 2016 , ' Dietary fat drives whole-body insulin resistance and promotes intestinal inflammation independent of body weight gain ' , Metabolism , vol. 65 , no. 12 , pp. 1706-1719 .
Notes :
application/pdf, English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1022568229
Document Type :
Electronic Resource