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2. Combining human liver ECM with topographically featured electrospun scaffolds for engineering hepatic microenvironment.

3. Utilising an in silico model to predict outcomes in senescence-driven acute liver injury.

4. Exploiting in silico modelling to enhance translation of liver cell therapies from bench to bedside.

5. Senolytic treatment preserves biliary regenerative capacity lost through cellular senescence during cold storage.

6. Human biliary epithelial cells from discarded donor livers rescue bile duct structure and function in a mouse model of biliary disease.

7. Notch-IGF1 signaling during liver regeneration drives biliary epithelial cell expansion and inhibits hepatocyte differentiation.

8. Response differences of HepG2 and Primary Mouse Hepatocytes to morphological changes in electrospun PCL scaffolds.

9. Cellular Senescence in Liver Disease and Regeneration.

10. Epithelial Plasticity during Liver Injury and Regeneration.

11. Phenotype instability of hepatocyte-like cells produced by direct reprogramming of mesenchymal stromal cells.

12. Altered Peripheral Blood Monocyte Phenotype and Function in Chronic Liver Disease: Implications for Hepatic Recruitment and Systemic Inflammation.

13. CRIg-expressing peritoneal macrophages are associated with disease severity in patients with cirrhosis and ascites.

14. Spatiotemporal Characterization of the Cellular and Molecular Contributors to Liver Fibrosis in a Murine Hepatotoxic-Injury Model.

15. Deletion of Wntless in myeloid cells exacerbates liver fibrosis and the ductular reaction in chronic liver injury.

16. Combining immunodetection with histochemical techniques: the effect of heat-induced antigen retrieval on picro-Sirius red staining.

17. The portal inflammatory infiltrate and ductular reaction in human nonalcoholic fatty liver disease.

18. Ductular reaction in hereditary hemochromatosis: the link between hepatocyte senescence and fibrosis progression.

19. Portal, but not lobular, macrophages express matrix metalloproteinase-9: association with the ductular reaction and fibrosis in chronic hepatitis C.

20. Macrophage secretory products induce an inflammatory phenotype in hepatocytes.

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