Apolipoprotein A-IV is induced by high-fat diets and mediates positive effects on glucose and lipid metabolism

Anne-Marie Lundsgaard, Rita Del Giudice, Josephine M Kanta, Mark Larance, Sarah L Armour, Amalie London, Michael M Richter, Nicoline R Andersen, Trine S Nicolaisen, Christian S Carl, Kim A Sjøberg, Kirstine Nyvold Bojsen-Møller, Jakob G Knudsen, Jens O Lagerstedt, Andreas M Fritzen, Bente Kiens*

*Corresponding author af dette arbejde
3 Citationer (Scopus)

Abstract

OBJECTIVE: Low-carbohydrate, high-fat diets under eucaloric conditions are associated with several health-beneficial metabolic effects in humans, particularly in the liver. We recently observed that apolipoprotein A-IV (apoA-IV), a highly abundant apolipoprotein, was among the most upregulated proteins in circulation after six weeks of consuming a high-fat diet in humans. However, the impact of dietary changes in regulating apoA-IV, and the potential effects of apoA-IV on regulation of glucose- and lipid metabolism remain to be fully established.

METHODS: We investigated the regulation of circulating fasting concentrations of apoA-IV in humans in response to diets enriched in either fat or carbohydrates. Moreover, to study the whole-body and tissue-specific glucose and lipid metabolic effects of apoA-IV, we administrered apoA-IV recombinant protein to mice and isolated pancreatic islets.

RESULTS: We demonstrate that in healthy human individuals high-fat intake increased fasting plasma apoA-IV concentrations by up to 54%, while high-carbohydrate intake suppressed plasma apoA-IV concentrations. In mice, administration of apoA-IV acutely lowered blood glucose levels both in lean and obese mice. Interestingly, this was related to a dual mechanism, involving both inhibition of hepatic glucose production and increased glucose uptake into white and brown adipose tissues. In addition to an effect on hepatic glucose production, the apoA-IV-induced liver proteome revealed increased capacity for lipoprotein clearance. The effects of apoA-IV in the liver and adipose tissues were concomitant with increased whole-body fatty acid oxidation. Upon glucose stimulation, an improvement in glucose tolerance by apoA-IV administration was related to potentiation of glucose-induced insulin secretion, while apoA-IV inhibited glucagon secretion ex vivo in islets.

CONCLUSIONS: We find that apoA-IV is potently increased by intake of fat in humans, and that several beneficial metabolic effects, previously associated with high fat intake in humans, are mimicked by administration of apoA-IV protein to mice.

OriginalsprogEngelsk
Artikelnummer102119
TidsskriftMolecular Metabolism
Vol/bind95
ISSN2212-8778
DOI
StatusUdgivet - maj 2025

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