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1. Intestinal gluconeogenesis controls the neonatal development of hypothalamic feeding circuits

2. Normalization of hepatic ChREBP activity does not protect against liver disease progression in a mouse model for Glycogen Storage Disease type Ia

3. A caveolin-1 dependent glucose-6-phosphatase trafficking contributes to hepatic glucose production

4. Increased atherosclerosis in a mouse model of glycogen storage disease type 1a

5. mRNA therapy restores euglycemia and prevents liver tumors in murine model of glycogen storage disease

6. Pathogenesis of Hepatic Tumors following Gene Therapy in Murine and Canine Models of Glycogen Storage Disease

7. Hepatocyte-specific glucose-6-phosphatase deficiency disturbs platelet aggregation and decreases blood monocytes upon fasting-induced hypoglycemia

8. Hepatic stress associated with pathologies characterized by disturbed glucose production

9. The role of kidney in the inter-organ coordination of endogenous glucose production during fasting

10. Intracellular lipids are an independent cause of liver injury and chronic kidney disease in non alcoholic fatty liver disease-like context

11. Glucose-6 Phosphate, A Central Hub for Liver Carbohydrate Metabolism

12. In vivo hepatic lipid quantification using MRS at 7 Tesla in a mouse model of glycogen storage disease type 1a

13. Mechanisms by Which Metabolic Reprogramming in GSD1 Liver Generates a Favorable Tumorigenic Environment

14. A hypometabolic defense strategy against malaria

15. Hepatic Carbohydrate Response Element Binding Protein Activation Limits Nonalcoholic Fatty Liver Disease Development in a Mouse Model for Glycogen Storage Disease Type 1a

16. A novel therapeutic strategy for skeletal disorders: Proof of concept of gene therapy for X-linked hypophosphatemia

17. Intestinal Gluconeogenesis Regulates Brown and White Adipose Tissues Functions in mice

18. La néoglucogenèse intestinale active la thermogenèse du tissu adipeux brun en mobilisant le système nerveux sympathique

19. Hepatocyte-specific glucose-6-phosphatase deficiency disturbs platelet aggregation and decreases blood monocytes upon fasting-induced hypoglycemia

20. Glucose-6-Phosphate Regulates Hepatic Bile Acid Synthesis in Mice

21. Tamoxifen Treatment in the Neonatal Period Affects Glucose Homeostasis in Adult Mice in a Sex-Dependent Manner

22. mRNA therapy restores euglycemia and prevents liver tumors in murine model of glycogen storage disease

23. Impaired Very-Low-Density Lipoprotein catabolism links hypoglycemia to hypertriglyceridemia in Glycogen Storage Disease type Ia

24. AAV liver gene therapy-mediated inhibition of FGF23 signaling as a therapeutic strategy for X-linked hypophosphatemia

25. Intestinal gluconeogenesis and protein diet: future directions

26. Intestinal gluconeogenesis prevents obesity-linked liver steatosis and non-alcoholic fatty liver disease

27. Glycogen storage disease type 1a is associated with disturbed vitamin A metabolism and elevated serum retinol levels

28. La NGI protège des altérations du métabolisme du tissu adipeux associées à l’obésité

29. Dietary exacerbation of metabolic stress leads to accelerated hepatic carcinogenesis in glycogen storage disease type Ia

30. Pathogenesis of Hepatic Tumors following Gene Therapy in Murine and Canine Models of Glycogen Storage Disease

31. Inhibition of Glycogen Synthase II with RNAi Prevents Liver Injury in Mouse Models of Glycogen Storage Diseases

32. Cibler le foie, des glycogénoses à la stéatose hépatique non alcoolique

33. Challenges of Gene Therapy for the Treatment of Glycogen Storage Diseases Type I and Type III

34. Mechanisms by Which Metabolic Reprogramming in GSD1 Liver Generates a Favorable Tumorigenic Environment

35. Contributors

36. Master role of glucose-6-phosphate in cell signaling and consequences of its deregulation in the liver and kidneys

37. Progressive development of renal cysts in glycogen storage disease type I

38. Rescue of GSDIII Phenotype with Gene Transfer Requires Liver- and Muscle-Targeted GDE Expression

39. G6PC mRNA Therapy Positively Regulates Fasting Blood Glucose and Decreases Liver Abnormalities in a Mouse Model of Glycogen Storage Disease 1a

40. Polycystic kidney features of the renal pathology in glycogen storage disease type I: possible evolution to renal neoplasia

41. Hepatocytes contribute to residual glucose production in a mouse model for glycogen storage disease type Ia

42. Clinical and biochemical heterogeneity between patients with glycogen storage disease type IA: the added value of CUSUM for metabolic control

43. Metabolic Adaptation Establishes Disease Tolerance to Sepsis

44. Gut-Brain Glucose Signaling in Energy Homeostasis

45. Adaptation of Hepatic, Renal and Intestinal Gluconeogenesis During Food Deprivation

46. Lessons from new mouse models of glycogen storage disease type 1a in relation to the time course and organ specificity of the disease

49. Glycogen storage disease type 1 and diabetes: Learning by comparing and contrasting the two disorders

50. Liver PPARα is crucial for whole-body fatty acid homeostasis and is protective against NAFLD

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