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Merck
  • Single-pass intestinal perfusion to establish the intestinal permeability of model drugs in mouse.

Single-pass intestinal perfusion to establish the intestinal permeability of model drugs in mouse.

International journal of pharmaceutics (2012-07-21)
Elvira Escribano, Xavier García Sala, Jorge Salamanca, Claudia Roig Navarro, Josep Queralt Regué
摘要

The aim of the present work was to study the intestinal permeabilities (P(eff)) of five model drugs: furosemide, piroxicam, naproxen, ranitidine and amoxicillin in the in situ intestinal perfusion technique in mice and compare them with corresponding rat and human in vivo P(eff) values. The main experimental conditions were: mice CD1 30-35 g, test drug concentrations in perfusion experiments (the highest dose strength dissolved in 250 mL of PBS pH 6.2) and flow rate of 0.2 mL/min. The test compounds were assayed following a validated HPLC method. The effective permeability coefficients at steady-state were calculated after correcting the outlet concentration following the gravimetric correction method proposed by Sutton et al. (2001). The permeability coefficient values ranged from 0.1751±0.0756×10(-4) cm/s for ranitidine to 17.19±4.16×10(-4) cm/s for naproxen. The mouse method correctly assigned the BCS permeability classification of a given drug and a correlation between mouse permeability data and the fraction of an oral dose absorbed in humans was achieved (FA=1-exp(-34,745·P(eff(mouse))); R=0.9631). Based on the results obtained, we conclude that mouse can be considered a valuable tool in the evaluation of intestinal permeability in order to predict the extent of human gastrointestinal absorption following oral administration of a drug.

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Sigma-Aldrich
雷尼替丁 盐酸盐, solid
Supelco
雷尼替丁 盐酸盐, Pharmaceutical Secondary Standard; Certified Reference Material