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1. Human liver organoids: From generation to applications.

2. FXR Isoforms Control Different Metabolic Functions in Liver Cells via Binding to Specific DNA Motifs.

3. Farnesoid X receptor and bile acids regulate vitamin A storage.

4. Steroidogenic control of liver metabolism through a nuclear receptor-network.

5. Farnesoid X receptor: A "homeostat" for hepatic nutrient metabolism.

6. Farnesoid X Receptor Activation Promotes Hepatic Amino Acid Catabolism and Ammonium Clearance in Mice.

7. Characterization of stem cell-derived liver and intestinal organoids as a model system to study nuclear receptor biology.

8. Quantitative liver proteomics identifies FGF19 targets that couple metabolism and proliferation.

9. Gene expression profiling in human precision cut liver slices in response to the FXR agonist obeticholic acid.

10. Raised hepatic bile acid concentrations during pregnancy in mice are associated with reduced farnesoid X receptor function.

11. The normal mechanisms of pregnancy-induced liver growth are not maintained in mice lacking the bile acid sensor Fxr.

12. Intestinal detoxification limits the activation of hepatic pregnane X receptor by lithocholic acid.

13. Farnesoid X Receptor Activation Promotes Hepatic Amino Acid Catabolism and Ammonium Clearance in Mice

14. Farnesoid X Receptor as a homeostat for hepatic nutrient metabolism, proliferation and intestinal inflammation : Novel insights into mechanisms of regulation

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