4.3 Article

Formulation and Evaluation of a Self-microemulsifying Drug Delivery System Containing Bortezomib

期刊

CHEMICAL & PHARMACEUTICAL BULLETIN
卷 64, 期 8, 页码 1108-1117

出版社

PHARMACEUTICAL SOC JAPAN
DOI: 10.1248/cpb.c16-00035

关键词

bortezomib; labrasol; microemulsion; self-microemulsifying drug delivery system (SMEDDS); pharmacokinetics

资金

  1. Ministry for Health, Welfare & Family Affairs, Republic of Korea [A092018]
  2. Handok Inc. (Seoul, Korea)

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The purposes of the present study were to develop a self-microemulsifying drug delivery system (SMEDDS) containing bortezomib, a proteasome inhibitor. The solubility of the drug was evaluated in 15 pharmaceutical excipients. Combinations of oils, surfactants and cosurfactants were screened by drawing pseudo-ternary phase diagrams. The system exhibiting the largest region of microemulsion was considered optimal. Bortezomib SMEDDS spontaneously formed a microemulsion when diluted with an aqueous medium with a median droplet size of approximately 20-30 nm. In vitro release studies showed that the SMEDDS had higher initial release rates for the drug when compared with the raw drug material alone. Measurement of the viscosity, size, and ion conductivity indicated that a phase inversion from water in an oil system to oil in a water system occurred when the weight ratio of the water exceeded 30% of the entire microemulsion system. In a pharmacokinetics study using rats, the bortezomib microemulsion failed to improve the bioavailability of the drug. The reason was assumed to be degradation of the drug in the microemulsion in the gastrointestinal tract. However, bortezomib in Labrasol (R) solution (an aqueous solution containing 0.025% Labraso (R)) showed significantly increased area under the curve from 0-24h (AUC(0-24h)) and maximum plasma concentration (C-max) values compared to the drug suspension. The findings of this study imply that oral delivery of a bortezomib and colloidal system containing Labrasol (R) could be an effective strategy for the delivery of bortezomib.

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