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70 results on '"Amodiaquine metabolism"'

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1. Amodiaquine Nonspecifically Binds Double Stranded and Three-Way Junction DNA Structures.

2. Exploring the repositioning of the amodiaquine as potential drug against visceral leishmaniasis: The in vitro effect against Leishmania infantum is associated with multiple mechanisms, involving mitochondria dysfunction, oxidative stress and loss of cell cycle control.

3. Assessment of NR4A Ligands That Directly Bind and Modulate the Orphan Nuclear Receptor Nurr1.

4. Beneficial Effect of Chloroquine and Amodiaquine on Type 1 Diabetic Tubulopathy by Attenuating Mitochondrial Nox4 and Endoplasmic Reticulum Stress.

5. Synthesis of stable isotope-labeled chloroquine and amodiaquine and their metabolites.

6. A novel cytochrome P450 mono-oxygenase from Streptomyces platensis resembles activities of human drug metabolizing P450s.

7. New phenylaniline derivatives as modulators of amyloid protein precursor metabolism.

8. Deconstructing Quinoline-Class Antimalarials to Identify Fundamental Physicochemical Properties of Beta-Hematin Crystal Growth Inhibitors.

9. Human glutathione S-transferases- and NAD(P)H:quinone oxidoreductase 1-catalyzed inactivation of reactive quinoneimines of amodiaquine and N-desethylamodiaquine: Possible implications for susceptibility to amodiaquine-induced liver toxicity.

10. The effect of milk thistle (Silybum marianum) and its main flavonolignans on CYP2C8 enzyme activity in human liver microsomes.

11. Influence of LAR and VAR on Para-Aminopyridine Antimalarials Targetting Haematin in Chloroquine-Resistance.

12. Nuclear receptor Nurr1 agonists enhance its dual functions and improve behavioral deficits in an animal model of Parkinson's disease.

13. Inhibitory effect of six herbal extracts on CYP2C8 enzyme activity in human liver microsomes.

14. Interactions of the antimalarial amodiaquine with lipid model membranes.

15. Involvement of myeloperoxidase and NADPH oxidase in the covalent binding of amodiaquine and clozapine to neutrophils: implications for drug-induced agranulocytosis.

16. Heat stabilization of blood spot samples for determination of metabolically unstable drug compounds.

17. In-vitro inhibitory effect of Tualang honey on cytochrome P450 2C8 activity.

18. Investigation of the interaction between amodiaquine and human serum albumin by fluorescence spectroscopy and molecular modeling.

19. Confirmation of Frm2 as a novel nitroreductase in Saccharomyces cerevisiae.

20. Distribution of human CYP2C8*2 allele in three different African populations.

21. Gene, ethnic and gender influences predisposition of adverse drug reactions to artesunate among Malaysians.

22. A ferrocene-based reagent for the conjugation and quantification of reactive metabolites.

23. Enhanced screening of glutathione-trapped reactive metabolites by in-source collision-induced dissociation and extraction of product ion using UHPLC-high resolution mass spectrometry.

24. Species differences in intestinal metabolic activities of cytochrome P450 isoforms between cynomolgus monkeys and humans.

25. Cytochrome P450 enzymes and genotype-guided drug therapy.

26. A microfluidic chip for electrochemical conversions in drug metabolism studies.

27. Field-adapted sampling of whole blood to determine the levels of amodiaquine and its metabolite in children with uncomplicated malaria treated with amodiaquine plus artesunate combination.

28. Novel metabolites of amodiaquine formed by CYP1A1 and CYP1B1: structure elucidation using electrochemistry, mass spectrometry, and NMR.

29. Covalent protein modification by reactive drug metabolites using online electrochemistry/liquid chromatography/mass spectrometry.

30. Effect of concomitant artesunate administration and cytochrome P4502C8 polymorphisms on the pharmacokinetics of amodiaquine in Ghanaian children with uncomplicated malaria.

31. Amodiaquine pharmacogenetics.

32. Determination of N-desethylamodiaquine by hydrophilic interaction liquid chromatography with tandem mass spectrometry: application to in vitro drug metabolism studies.

33. Amodiaquine metabolism is impaired by common polymorphisms in CYP2C8: implications for malaria treatment in Africa.

34. Heterotropic and homotropic cooperativity by a drug-metabolising mutant of cytochrome P450 BM3.

35. [Cytochrome P-450 and the response to antimalarial drugs].

36. Structural basis for inhibition of histamine N-methyltransferase by diverse drugs.

37. Pharmacodynamic interactions of amodiaquine and its major metabolite desethylamodiaquine with artemisinin, quinine and atovaquone in Plasmodium falciparum in vitro.

38. CYP2C8 polymorphism frequencies among malaria patients in Zanzibar.

39. Short report: lack of prediction of amodiaquine efficacy in treating Plasmodium falciparum malaria by in vitro tests.

40. Influence of amodiaquine treatment on microsomal lipid peroxidation and antioxidant defense systems of rats.

41. Interaction of chloroquine and its analogues with heme: An isothermal titration calorimetric study.

42. Central role of hemoglobin degradation in mechanisms of action of 4-aminoquinolines, quinoline methanols, and phenanthrene methanols.

43. 4-Aminoquinoline resistance of Plasmodium falciparum: insights from the study of amodiaquine uptake.

44. Amodiaquine accumulation in Plasmodium falciparum as a possible explanation for its superior antimalarial activity over chloroquine.

45. Mouse liver nicotinamide N-methyltransferase pharmacogenetics: biochemical properties and variation in activity among inbred strains.

46. The bioactivation of amodiaquine by human polymorphonuclear leucocytes in vitro: chemical mechanisms and the effects of fluorine substitution.

47. The effect of chemical substitution on the metabolic activation, metabolic detoxication, and pharmacological activity of amodiaquine in the mouse.

48. Role of hepatic metabolism in the bioactivation and detoxication of amodiaquine.

49. The effect of fluorine substitution on the metabolism and antimalarial activity of amodiaquine.

50. Pharmacokinetic and pharmacodynamic study of amodiaquine and its two metabolites after a single oral dose in human volunteers.

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