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1. The global burden of cancer attributable to risk factors, 2010-19: a systematic analysis for the Global Burden of Disease Study 2019

2. Niclosamide reduces glucagon sensitivity via hepatic PKA inhibition in obese mice: Implications for glucose metabolism improvements in type 2 diabetes

3. Niclosamide blocks glucagon phosphorylation of Ser552 on β-catenin in primary rat hepatocytes via PKA signalling

4. The phosphoinositide 3'-kinase p110d modulates contractile protein production and IL-6 release in human airway smooth muscle

6. Comparison of growth factor signalling pathway utilisation in cultured normal melanocytes and melanoma cell lines

7. Insights into the role of JAK2-I724T variant in myeloproliferative neoplasms from a unique cohort of New Zealand patients.

8. A Polynesian-specific SLC22A3 variant associates with low plasma lipoprotein(a) concentrations independent of apo(a) isoform size in males.

9. Conditional Deletion of β-Catenin in the Mediobasal Hypothalamus Impairs Adaptive Energy Expenditure in Response to High-Fat Diet and Exacerbates Diet-Induced Obesity.

10. Evidence that RXFP4 is located in enterochromaffin cells and can regulate production and release of serotonin.

11. A role for β-catenin in diet-induced skeletal muscle insulin resistance.

12. Stratified glucose-lowering response to vildagliptin and pioglitazone by obesity and hypertriglyceridemia in a randomized crossover trial.

13. Response to BRAF-targeted Therapy Is Enhanced by Cotargeting VEGFRs or WNT/β-Catenin Signaling in BRAF-mutant Colorectal Cancer Models.

14. β-Cells retain a pool of insulin-containing secretory vesicles regulated by adherens junctions and the cadherin-binding protein p120 catenin.

15. The Impact of Exogenous Insulin Input on Calculating Hepatic Clearance Parameters.

16. Variability in Estimated Modelled Insulin Secretion.

17. The minor allele of the CREBRF rs373863828 p.R457Q coding variant is associated with reduced levels of myostatin in males: Implications for body composition.

18. Limited Metabolic Effect of the CREBRF R457Q Obesity Variant in Mice.

19. The CREBRF diabetes-protective rs373863828-A allele is associated with enhanced early insulin release in men of Māori and Pacific ancestry.

20. β-Catenin is required for optimal exercise- and contraction-stimulated skeletal muscle glucose uptake.

21. Glucose regulates expression of pro-inflammatory genes, IL-1β and IL-12, through a mechanism involving hexosamine biosynthesis pathway-dependent regulation of α-E catenin.

22. Diverse mechanisms activate the PI 3-kinase/mTOR pathway in melanomas: implications for the use of PI 3-kinase inhibitors to overcome resistance to inhibitors of BRAF and MEK.

23. Efficacy of Providing the PI3K p110α Inhibitor BYL719 (Alpelisib) to Middle-Aged Mice in Their Diet.

24. β-catenin regulates muscle glucose transport via actin remodelling and M-cadherin binding.

25. Prolonged treatment with a PI3K p110α inhibitor causes sex- and tissue-dependent changes in antioxidant content, but does not affect mitochondrial function.

26. Derivation of induced pluripotent stem cell lines from New Zealand donors.

27. Cetuximab produced from a goat mammary gland expression system is equally efficacious as innovator cetuximab in animal cancer models.

28. How does the duration of consults vary for upper respiratory tract infections in general practice where an antibiotic has been prescribed?

29. The CSF1 receptor inhibitor pexidartinib (PLX3397) reduces tissue macrophage levels without affecting glucose homeostasis in mice.

30. Orthogonal assays for the identification of inhibitors of the single-stranded nucleic acid binding protein YB-1.

31. For Better or Worse: The Potential for Dose Limiting the On-Target Toxicity of PI 3-Kinase Inhibitors.

32. Identification, structure modification, and characterization of potential small-molecule SGK3 inhibitors with novel scaffolds.

33. Macrophages enhance Vegfa-driven angiogenesis in an embryonic zebrafish tumour xenograft model.

34. High-throughput screening campaigns against a PI3Kα isoform bearing the H1047R mutation identified potential inhibitors with novel scaffolds.

35. Discordant association of the CREBRF rs373863828 A allele with increased BMI and protection from type 2 diabetes in Māori and Pacific (Polynesian) people living in Aotearoa/New Zealand.

37. The role of adherens junction proteins in the regulation of insulin secretion.

38. Biological characterization of SN32976, a selective inhibitor of PI3K and mTOR with preferential activity to PI3Kα, in comparison to established pan PI3K inhibitors.

39. Niclosamide reduces glucagon sensitivity via hepatic PKA inhibition in obese mice: Implications for glucose metabolism improvements in type 2 diabetes.

40. A Critical Role for β-Catenin in Modulating Levels of Insulin Secretion from β-Cells by Regulating Actin Cytoskeleton and Insulin Vesicle Localization.

41. NRAS and EPHB6 mutation rates differ in metastatic melanomas of patients in the North Island versus South Island of New Zealand.

42. Inhibitors of pan-PI3K Signaling Synergize with BRAF or MEK Inhibitors to Prevent BRAF-Mutant Melanoma Cell Growth.

43. Targeting class IA PI3K isoforms selectively impairs cell growth, survival, and migration in glioblastoma.

44. Hypothalamic WNT signalling is impaired during obesity and reinstated by leptin treatment in male mice.

45. Enzyme activity effects of N-terminal His-tag attached to catalytic sub-unit of phosphoinositide-3-kinase.

46. Extended treatment with selective phosphatidylinositol 3-kinase and mTOR inhibitors has effects on metabolism, growth, behaviour and bone strength.

47. Cholesterol-induced mammary tumorigenesis is enhanced by adiponectin deficiency: role of LDL receptor upregulation.

48. Oncogenic mutations of p110α isoform of PI 3-kinase upregulate its protein kinase activity.

49. Protein kinase activity of phosphoinositide 3-kinase regulates cytokine-dependent cell survival.

50. Concurrent resistance and aerobic exercise stimulates both myofibrillar and mitochondrial protein synthesis in sedentary middle-aged men.

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