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13. In vivo evaluation of acute intravenous toxicity of a [Ga-68]Ga-PSMA-11-microemulsion

14. Development and evaluation of a reconstitutable dry suspension containing isoniazid for flexible pediatric dosing

15. Development and validation of an LC-MS/MS method for the quantification of goserelin in a Pheroid (R) formulation, in simulated intestinal fluid

17. A resource of targeted mutant mouse lines for 5,061 genes

18. Comparison of drug transporter gene expression and functionality in Caco-2 cells from 10 different laboratories

20. Co-administration of African potato and cisplatin for treating breast and prostate cancers using a Pheroid® delivery system

26. Co-administration of African potato and cisplatin for treatingbreast and prostate cancers using a Pheroid® delivery system

27. Establishment and characterization of allograft and xenograft cancer rodent models

28. The effect of entrapment of a peptide in Pheroid® on pharmacokinetics and testosterone levels

29. Evaluation of the oral delivery of a peptide with Pheroid® technology

31. Functionalization of PLGA nanoparticles with 1,3-β-glucan enhances the intracellular pharmacokinetics of rifampicin in macrophages

34. The fabrication and characterization of a PLGA nanoparticle–Pheroid® combined drug delivery system

36. Spray-Dried, Nanoencapsulated, Multi-Drug Anti-Tuberculosis Therapy Aimed at Once Weekly Administration for the Duration of Treatment

37. Bioaccumulation and subchronic toxicity of 14 nm gold nanoparticles in rats

38. Oral lipid-based nanoformulation of tafenoquine enhanced bioavailability and blood stage antimalarial efficacy and led to a reduction in human red blood cell loss in mice

42. Oral lipid-based nanoformulation of tafenoquine enhanced bioavailability and blood stage antimalarial efficacy and led to a reduction in human red blood cell loss in mice

43. The fabrication and characterization of a PLGA nanoparticle-Pheroid combined drug delivery system.

44. Oral lipid-based nanoformulation of tafenoquine enhanced bioavailability and blood stage antimalarial efficacy and led to a reduction in human red blood cell loss in mice

45. Effects of protein binding on the biodistribution of PEGylated PLGA nanoparticles post oral administration

46. Nanoparticle Formulation of a Poorly Soluble Cannabinoid Receptor 1 Antagonist Improves Absorption by Rat and Human Intestine

47. Permeation of PLGA Nanoparticles Across Different in vitro Models

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