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1. Comparative Evaluation of Dissolution Performance in a USP 2 Setup and Alternative Stirrers and Vessel Designs: A Systematic Computational Investigation

2. In Vitro Predictive Dissolution Test Should Be Developed and Recommended as a Bioequivalence Standard for the Immediate-Release Solid Oral Dosage Forms of the Highly Variable Mycophenolate Mofetil

3. Improving Dissolution Behavior and Oral Absorption of Drugs with pH-Dependent Solubility Using pH Modifiers: A Physiologically Realistic Mass Transport Analysis

5. Hierarchical Mass Transfer Analysis of Drug Particle Dissolution, Highlighting the Hydrodynamics, pH, Particle Size, and Buffer Effects for the Dissolution of Ionizable and Nonionizable Drugs in a Compendial Dissolution Vessel

6. Ultrathin, Large-Area Membrane Diffusion Cell for pH-Dependent Simultaneous Dissolution and Absorption Studies

7. Chemoproteomic Identification of Serine Hydrolase RBBP9 as a Valacyclovir-Activating Enzyme

8. Mass Transport Analysis of Bicarbonate Buffer: Effect of the CO2–H2CO3Hydration–Dehydration Kinetics in the Fluid Boundary Layer and the Apparent Effective pKaControlling Dissolution of Acids and Bases

9. Mass Transport Analysis of the Enhanced Buffer Capacity of the Bicarbonate–CO2Buffer in a Phase-Heterogenous System: Physiological and Pharmaceutical Significance

10. Linking the Gastrointestinal Behavior of Ibuprofen with the Systemic Exposure between and within Humans—Part 2: Fed State

11. Linking the Gastrointestinal Behavior of Ibuprofen with the Systemic Exposure between and within Humans—Part 1: Fasted State Conditions

12. Pulse Packet Stochastic Model for Gastric Emptying in the Fasted State: A Physiological Approach

13. Improved Protease-Targeting and Biopharmaceutical Properties of Novel Prodrugs of Ganciclovir

14. In Vitro Characterization of the Biomimetic Properties of Poly(dimethylsiloxane) To Simulate Oral Drug Absorption

15. In VivoDissolution and Systemic Absorption of Immediate Release Ibuprofen in Human Gastrointestinal Tract under Fed and Fasted Conditions

16. Low Buffer Capacity and Alternating Motility along the Human Gastrointestinal Tract: Implications for in VivoDissolution and Absorption of Ionizable Drugs

17. Magnetic Resonance Imaging Quantification of Fasted State Colonic Liquid Pockets in Healthy Humans

18. Utilization of Gastrointestinal Simulator, an in Vivo Predictive Dissolution Methodology, Coupled with Computational Approach To Forecast Oral Absorption of Dipyridamole

19. Measurement of in vivoGastrointestinal Release and Dissolution of Three Locally Acting Mesalamine Formulations in Regions of the Human Gastrointestinal Tract

20. Mechanistic Analysis of Cocrystal Dissolution as a Function of pH and Micellar Solubilization

21. Particle Size, Dose, and Confinement Affect Passive Diffusion Flux through the Membrane Concentration Boundary Layer

22. Gastrointestinal Motility Variation and Implications for Plasma Level Variation: Oral Drug Products

23. Substrate-Competitive Activity-Based Profiling of Ester Prodrug Activating Enzymes

24. In VitroDissolution of Fluconazole and Dipyridamole in Gastrointestinal Simulator (GIS), Predicting in VivoDissolution and Drug–Drug Interaction Caused by Acid-Reducing Agents

25. Intestinal Permeability Study of Minoxidil: Assessment of Minoxidil as a High Permeability Reference Drug for Biopharmaceutics Classification

26. Dipeptidyl Peptidase IV as a Potential Target for Selective Prodrug Activation and Chemotherapeutic Action in Cancers

27. Quantification of Gastrointestinal Liquid Volumes and Distribution Following a 240 mL Dose of Water in the Fasted State

28. The Low/High BCS Permeability Class Boundary: Physicochemical Comparison of Metoprolol and Labetalol

29. Ion Pairing with Bile Salts Modulates Intestinal Permeability and Contributes to Food–Drug Interaction of BCS Class III Compound Trospium Chloride

30. Purely in Silico BCS Classification: Science Based Quality Standards for the World’s Drugs

31. Mechanistic Understanding of Food Effects: Water Diffusivity in Gastrointestinal Tract Is an Important Parameter for the Prediction of Disintegration of Solid Oral Dosage Forms

32. Establishing the Pharmaceutical Quality of Chinese Herbal Medicine: A Provisional BCS Classification

33. Cytomegalovirus Protease Targeted Prodrug Development

34. Comparison of the Permeability of Metoprolol and Labetalol in Rat, Mouse, and Caco-2 Cells: Use as a Reference Standard for BCS Classification

35. Increasing Oral Absorption of Polar Neuraminidase Inhibitors: A Prodrug Transporter Approach Applied to Oseltamivir Analogue

36. The Fraction Dose Absorbed, in Humans, and High Jejunal Human Permeability Relationship

37. Provisional Biopharmaceutical Classification of Some Common Herbs Used in Western Medicine

38. Enhancing the Intestinal Membrane Permeability of Zanamivir: A Carrier Mediated Prodrug Approach

39. The Solubility–Permeability Interplay: Mechanistic Modeling and Predictive Application of the Impact of Micellar Solubilization on Intestinal Permeation

40. Mechanistic enhancement of the intestinal absorption of drugs containing the polar guanidino functionality

41. Specificity of a Prodrug-Activating Enzyme hVACVase: The Leaving Group Effect

42. Physiological Parameters for Oral Delivery and in VitroTesting

43. High-Permeability Criterion for BCS Classification: Segmental/pH Dependent Permeability Considerations

44. The Biowaiver Extension for BCS Class III Drugs: The Effect of Dissolution Rate on the Bioequivalence of BCS Class III Immediate-Release Drugs Predicted by Computer Simulation

45. Enabling the Intestinal Absorption of Highly Polar Antiviral Agents: Ion-Pair Facilitated Membrane Permeation of Zanamivir Heptyl Ester and Guanidino Oseltamivir

46. Chemical and Enzymatic Stability of Amino Acid Prodrugs Containing Methoxy, Ethoxy and Propylene Glycol Linkers

47. Multiple Efflux Pumps Are Involved in the Transepithelial Transport of Colchicine: Combined Effect of P-Glycoprotein and Multidrug Resistance-Associated Protein 2 Leads to Decreased Intestinal Absorption Throughout the Entire Small Intestine

48. Toward an In VivoDissolution Methodology: A Comparison of Phosphate and Bicarbonate Buffers

49. Segmental Dependent Transport of Low Permeability Compounds along the Small Intestine Due to P-Glycoprotein: The Role of Efflux Transport in the Oral Absorption of BCS Class III Drugs

50. Characteristics of Gastrointestinal Absorption of DX-9065a, a New Synthetic Anticoagulant

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