Afficher la couverture 'Insights from liver‐humanized mice on cholesterol lipoprotein metabolism and LXR‐agonist pharmacodynamics in humans | Minniti, Mirko' en grand format
/5

0 avis

Insights from liver‐humanized mice on cholesterol lipoprotein metabolism and LXR‐agonist pharmacodynamics in humans

Archive ouverte

Minniti, Mirko | Pedrelli, Matteo | Vedin, Lise‐lotte | Delbès, Anne‐sophie | Denis, Raphaël G.P. | Öörni, Katariina | Sala, Claudia | Pirazzini, Chiara | Thiagarajan, Divya | Nurmi, Harri | Grompe, Markus | Mills, Kevin | Garagnani, Paolo | Ellis, Ewa C.S. | Strom, Stephen | Luquet, Serge | Wilson, Elizabeth | Bial, John | Steffensen, Knut | Parini, Paolo

Edité par CCSD ; Wiley-Blackwell -

International audience. Background and Aims; Genetically modified mice have been used extensively to study human disease. However, the data gained are not always translatable to humans because of major species differences. Liver‐humanized mice (LHM) are considered a promising model to study human hepatic and systemic metabolism. Therefore, we aimed to further explore their lipoprotein metabolism and to characterize key hepatic species‐related, physiological differences.Approach and Results: Fah−/−, Rag2−/−, and Il2rg−/− knockout mice on the nonobese diabetic (FRGN) background were repopulated with primary human hepatocytes from different donors. Cholesterol lipoprotein profiles of LHM showed a human‐like pattern, characterized by a high ratio of low‐density lipoprotein to high‐density lipoprotein, and dependency on the human donor. This pattern was determined by a higher level of apolipoprotein B100 in circulation, as a result of lower hepatic mRNA editing and low‐density lipoprotein receptor expression, and higher levels of circulating proprotein convertase subtilisin/kexin type 9. As a consequence, LHM lipoproteins bind to human aortic proteoglycans in a pattern similar to human lipoproteins. Unexpectedly, cholesteryl ester transfer protein was not required to determine the human‐like cholesterol lipoprotein profile. Moreover, LHM treated with GW3965 mimicked the negative lipid outcomes of the first human trial of liver X receptor stimulation (i.e., a dramatic increase of cholesterol and triglycerides in circulation). Innovatively, LHM allowed the characterization of these effects at a molecular level.Conclusions: LHM represent an interesting translatable model of human hepatic and lipoprotein metabolism. Because several metabolic parameters displayed donor dependency, LHM may also be used in studies for personalized medicine.

Suggestions

Du même auteur

Soat2 ties cholesterol metabolism to β‐oxidation and glucose tolerance in male mice

Archive ouverte | Pramfalk, Camilla | CCSD

International audience. Background: Sterol O-acyltransferase 2 (Soat2) encodes acyl-coenzyme A:cholesterol acyltransferase 2 (ACAT2), which synthesizes cholesteryl esters in hepatocytes and enterocytes fated either ...

Mice with humanized livers reveal the role of hepatocyte clocks in rhythmic behavior

Archive ouverte | Delbès, Anne-Sophie | CCSD

International audience. The synchronization of circadian clock depends on a central pacemaker located in the suprachiasmatic nuclei. However, the potential feedback of peripheral signals on the central clock remains...

Mice with humanized livers reveal the involvement of hepatocyte circadian clocks in rhythmic behavior and physiology

Archive ouverte | Delbès, Anne-Sophie | CCSD

The circadian clock is an evolutionarily acquired gene network that synchronizes physiological processes to adapt homeostasis to the succession of day and night. While most mammalian cells have a circadian clock, their synchroniza...

Chargement des enrichissements...