PPAR gamma Modulates Long Chain Fatty Acid Processing in the Intestinal Epithelium



Duszka K, Oresic M, Le May C, König J, Wahli W

PublisherMDPI AG

2017

International Journal of Molecular Sciences

INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES

INT J MOL SCI

ARTN 2559

18

12

15

1422-0067

1422-0067

DOIhttps://doi.org/10.3390/ijms18122559

http://www.dx.doi.org/10.3390/ijms18122559

https://research.utu.fi/converis/portal/detail/Publication/29145043


Nuclear receptor PPAR gamma affects lipid metabolism in several tissues, but its role in intestinal lipid metabolism has not been explored. As alterations have been observed in the plasma lipid profile of ad libitum fed intestinal epithelium-specific PPAR gamma knockout mice (iePPAR gamma KO), we submitted these mice to lipid gavage challenges. Within hours after gavage with long chain unsaturated fatty acid (FA)-rich canola oil, the iePPAR gamma KO mice had higher plasma free FA levels and lower gastric inhibitory polypeptide levels than their wild-type (WT) littermates, and altered expression of incretin genes and lipid metabolism-associated genes in the intestinal epithelium. Gavage with the medium chain saturated FA-rich coconut oil did not result in differences between the two genotypes. Furthermore, the iePPAR gamma KO mice did not exhibit defective lipid uptake and stomach emptying; however, their intestinal transit was more rapid than in WT mice. When fed a canola oil-rich diet for 4.5 months, iePPAR gamma KO mice had higher body lean mass than the WT mice. We conclude that intestinal epithelium PPAR gamma is activated preferentially by long chain unsaturated FAs compared to medium chain saturated FAs. Furthermore, we hypothesize that the iePPAR gamma KO phenotype originates from altered lipid metabolism and release in epithelial cells, as well as changes in intestinal motility.

Last updated on 2024-26-11 at 15:08