4.6 Article

Lipid-core nanocapsules restrained the indomethacin ethyl ester hydrolysis in the gastrointestinal lumen and wall acting as mucoadhesive reservoirs

期刊

EUROPEAN JOURNAL OF PHARMACEUTICAL SCIENCES
卷 39, 期 1-3, 页码 116-124

出版社

ELSEVIER SCIENCE BV
DOI: 10.1016/j.ejps.2009.11.004

关键词

Indomethacin ethyl ester; Fluorescent-labeled polymer; Polyester; Lipid-core nanocapsules; Ex vivo and in vivo intestinal absorption

资金

  1. Centro de Nanociencia e Nanotecnologia - UFRGS
  2. CNPq/Brasilia/Brazil, FINEP/MCT
  3. Universal/CNPq
  4. Rede Nanocosmeticos CNPq/MCT
  5. IBSA/CNPq
  6. CAPES
  7. CAPES/COFECUB

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The aim of this work was to investigate if the indomethacin ethyl ester (IndOEt) released from lipid-core nanocapsules (NC) is converted into indomethacin (IndOH) in the intestine lumen, intestine wall OF after the particles reach the blood stream. NC-IndOEt had monomodal size distribution (242 nm; PDI 0.2) and zeta potential of -11 mV. The everted rat gut sac model showed IndOEt passage of 0.16 mu mol m(-2) through the serosal fluid (30 min). From 15 to 120 min, the IndOEt concentrations in the tissue increased from 6.13 to 27.47 mu mol m(-2). No IndOH was formed ex vivo. A fluorescent-NC formulation was used to determine the copolymer bioadhesion (0.012 mu mol m(-2)). After NC-IndOEt oral administration to rats, IndOEt and IndOH were detected in the gastrointestinal tract (contents and tissues). In the tissues, the IndOEt concentrations decreased from 459 to 5 mu g g(-1) after scrapping, demonstrating the NC mucoadhesion. In plasma (peripheric and portal vein), in spleen and liver, exclusively IndOH was detected. in conclusion, after oral closing of NC-IndOEt, IndOEt is converted into IndOH in the intestinal lumen and wall before reaching the blood stream. The complexity of a living system was not predicted by the ex vivo gut sac model. (C) 2009 Elsevier B.V. All rights reserved.

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