194 results on '"Pang, K S"'
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2. Pharmacokinetic Modeling of Drug Conjugates
3. Quantitative detection of engineered nanoparticles in tissues and organs: An investigation of efficacy and linear dynamic ranges using ICP-AES
4. ITC Recommendations for Transporter Kinetic Parameter Estimation and Translational Modeling of Transport-Mediated PK and DDIs in Humans
5. Pharmacokinetics of tranexamic acid in patients undergoing cardiac surgery with use of cardiopulmonary bypass
6. Transport of 5,5-diphenylbarbituric acid and its precursors and their effect on P-gp, MRP2 and CYP3A4 in Caco-2 and LS180 cells
7. Metabolism: Scaling-up from In Vitro to Organ and Whole Body
8. An expressive-arts-based life-death education program for the elderly: A qualitative study
9. An expressive-arts-based life-death education program for the elderly: A qualitative study.
10. Functional Integrity of the Chimeric (Humanized) Mouse Liver: Enzyme Zonation, Physiologic Spaces, and Hepatic Enzymes and Transporters
11. Metabolite Kinetics: The Segregated Flow Model for Intestinal and Whole Body Physiologically Based Pharmacokinetic Modeling to Describe Intestinal and Hepatic Glucuronidation of Morphine in Rats In Vivo
12. Physiologically-Based Pharmacokinetic-Pharmacodynamic Modeling of 1 ,25-Dihydroxyvitamin D3 in Mice
13. 1 ,25-Dihydroxyvitamin D3 Reduces Cerebral Amyloid- Accumulation and Improves Cognition in Mouse Models of Alzheimer's Disease
14. Pharmacokinetics of Nanoscale Quantum Dots: In Vivo Distribution, Sequestration, and Clearance in the Rat
15. Dynamics of arterial and portal venous flow interactions in perfused rat liver: an intravital microscopic study
16. Enalaprilat handling by the kidney: barrier-limited cell entry
17. Determinants of Metabolite Disposition
18. D2O as a substitute for 3H2O, as a reference indicator in liver multiple-indicator dilution studies
19. [14C]urea and 58Co-EDTA as reference indicators in hepatic multiple indicator dilution studies
20. Transfer of enalaprilat across rat liver cell membranes is barrier limited
21. Competing pathways in drug metabolism. I. Effect of input concentration on the conjugation of gentisamide in the once-through in situ perfused rat liver preparation.
22. Stereoselective glutathione conjugation and amidase-catalyzed hydrolysis of alpha-bromoisovalerylurea enantiomers in isolated rat hepatocytes.
23. Effect of protein binding on 4-methylumbelliferyl sulfate desulfation kinetics in perfused rat liver.
24. Esterases for enalapril hydrolysis are concentrated in the perihepatic venous region of the rat liver.
25. Renal handling of enalapril and enalaprilat: studies in the isolated red blood cell-perfused rat kidney.
26. Kinetics of metabolite formation and elimination in the perfused rat liver preparation: differences between the elimination of preformed acetaminophen and acetaminophen formed from phenacetin.
27. Aberrant Pharmacokinetics of harmol in the perfused rat liver preparation: sulfate and glucuronide conjugations.
28. Normal and retrograde perfusion to probe the zonal distribution of sulfation and glucuronidation activities of harmol in the perfused rat liver preparation.
29. Glycine conjugation activity of benzoic acid and its acinar localization in the perfused rat liver.
30. Demonstration of rapid entry and a cellular binding space for salicylamide in perfused rat liver: a multiple indicator dilution study.
31. Combined hepatic arterial-portal venous and hepatic arterial-hepatic venous perfusions to probe the abundance of drug metabolizing activities: perihepatic venous O-deethylation activity for phenacetin and periportal sulfation activity for acetaminophen in the once-through rat liver preparation.
32. Retrograde perfusion to probe the heterogeneous distribution of hepatic drug metabolizing enzymes in rats.
33. Metabolite kinetics: formation of acetaminophen from deuterated and nondeuterated phenacetin and acetanilide on acetaminophen sulfation kinetics in the perfused rat liver preparation.
34. Disposition of enalapril in the perfused rat intestine-liver preparation: absorption, metabolism and first-pass effect.
35. Alteration of transit time and direction of flow to probe the heterogeneous distribution of conjugating activities for harmol in the perfused rat liver preparation.
36. Stereoselectivity in glutathione conjugation and amidase-catalyzed hydrolysis of the 2-bromoisovalerylurea enantiomers in the single-pass perfused rat liver.
37. Kinetics of sequential metabolism. I. Formation and metabolism of oxazepam from nordiazepam and temazepam in the perfused murine liver.
38. Kinetics of sequential metabolism. II. Formation and metabolism of nordiazepam and oxazepam from diazepam in the perfused murine liver.
39. Effects of retrograde flow on measured blood volume, Disse space, intracellular water space and drug extraction in the perfused rat liver: characterization by the multiple indicator dilution technique.
40. Sequential metabolism of salicylamide exclusively to gentisamide 5-glucuronide and not gentisamide sulfate conjugates in single-pass in situ perfused rat liver.
41. Viability of the vascularly perfused, recirculating rat intestine and intestine-liver preparations
42. Transport, binding, and metabolism of sulfate conjugates in the liver
43. Poisoning by toxic plants in Hong Kong: a 15-year review.
44. Budd-Chiari syndrome secondary to toxic pyrrolizidine alkaloid exposure.
45. Implantation metastasis in a 13-year-old girl: a case report.
46. Absorption of benzoic acid in segmental regions of the vascularly perfused rat small intestine preparation.
47. Hepatic uptake and metabolism of benzoate: a multiple indicator dilution, perfused rat liver study.
48. Futile cycling of estrone sulfate and estrone in the recirculating perfused rat liver preparation.
49. Sulfation is rate limiting in the futile cycling between estrone and estrone sulfate in enriched periportal and perivenous rat hepatocytes.
50. The multiple indicator dilution method and its utility in risk assessment.
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