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1. Amyloid beta 42 alters cardiac metabolism and impairs cardiac function in male mice with obesity

2. Identification of appropriate biochemical parameters and cut points to detect Maturity Onset Diabetes of Young (MODY) in Asian Indians in a clinic setting

3. Prior degree and academic performance in medical school: evidence for prioritising health students and moving away from a bio-medical science-focused entry stream

4. Copper Ionophores as Novel Antiobesity Therapeutics

5. Prevalence, clinical features and complications of common forms of Maturity Onset Diabetes of the Young (MODY) seen at a tertiary diabetes centre in south India

7. Amyloid beta 42 alters cardiac metabolism and impairs cardiac function in obesity

8. Cytokine‐inducible SH2 domain containing protein contributes to regulation of adiposity, food intake, and glucose metabolism

9. Advanced Glycation End-Products and Their Effects on Gut Health

10. Class IIa HDACs do not influence beta-cell function under normal or high glucose conditions

11. Copper Ionophores as Novel Antiobesity Therapeutics

12. Metformin, beta-cell development, and novel processes following beta-cell ablation in zebrafish

13. Scriptaid enhances skeletal muscle insulin action and cardiac function in obese mice

14. Clinical features, complications and treatment of rarer forms of maturity-onset diabetes of the young (MODY) - A review

15. Quality of Life and Diabetes in India: A scoping review

16. Development of an Innovative Screening Tool and Identification of Novel ß-Cell Protective Drugs

17. Adipocytokines as features of the metabolic syndrome determined using confirmatory factor analysis

18. Matrix Metalloproteinase-9 Reduces Islet Amyloid Formation by Degrading Islet Amyloid Polypeptide

19. One year of sitagliptin treatment protects against islet amyloid-associated ß-cell loss and does not induce pancreatitis or pancreatic neoplasia in mice

20. Scriptaid enhances skeletal muscle insulin action and cardiac function in obese mice

21. Gene expression signature: a powerful approach for drug discovery in diabetes

22. Pathways of Acetyl-CoA Metabolism Involved in the Reversal of Palmitate-Induced Glucose Production by Metformin and Salicylate

23. cJUN N-terminal kinase (JNK) activation mediates islet amyloid-induced beta cell apoptosis in cultured human islet amyloid polypeptide transgenic mouse islets

24. β-Cell Loss and β-Cell Apoptosis in Human Type 2 Diabetes Are Related to Islet Amyloid Deposition

25. Amyloid formation in human IAPP transgenic mouse islets and pancreas, and human pancreas, is not associated with endoplasmic reticulum stress

26. Amyloid formation results in recurrence of hyperglycaemia following transplantation of human IAPP transgenic mouse islets

27. Fructose-1,6-Bisphosphatase Overexpression in Pancreatic β-Cells Results in Reduced Insulin Secretion

28. Too much of a good thing: why it is bad to stimulate the beta cell to secrete insulin

29. Investigational agents that protect pancreatic islet β-cells from failure

30. ROSIGLITAZONE TREATMENT DOES NOT DECREASE AMYLOID DEPOSITION IN TRANSPLANTED ISLETS FROM TRANSGENIC MICE EXPRESSING HUMAN ISLET AMYLOID POLYPEPTIDE

31. Exendin-4 increases islet amyloid deposition but offsets the resultant beta cell toxicity in human islet amyloid polypeptide transgenic mouse islets

32. Neprilysin impedes islet amyloid formation by inhibition of fibril formation rather than peptide degradation

33. Oxidative stress is induced by islet amyloid formation and time-dependently mediates amyloid-induced beta cell apoptosis

34. Fructose-1,6-bisphosphatase overexpression in pancreatic beta-cells results in reduced insulin secretion: a new mechanism for fat-induced impairment of beta-cell function

35. Increased nicotinamide nucleotide transhydrogenase levels predispose to insulin hypersecretion in a mouse strain susceptible to diabetes

36. Differential effect of inbred mouse strain (C57BL/6, DBA/2, 129T2) on insulin secretory function in response to a high fat diet

37. High glucose-induced impairment in insulin secretion is associated with reduction in islet glucokinase in a mouse model of susceptibility to islet dysfunction

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