Oligonucleotide transport in rat and human intestine Ussing chamber models

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Abstract

Cellular and intestinal absorption of naked oligonucleotides (ONs) is limited and still remains a developmental challenge. A previous report in the literature suggests that ON absorption occurs via a paracellular mechanism. The aim of this study was to test this hypothesis using rat and human intestine in a Ussing chamber and in Caco-2 cells. Transport of a 35S-labelled mixed backbone ON (MBO) across human or rat intestinal tissue or across Caco-2 cells was measured after a 2-h incubation in the presence or absence of increasing MBO concentrations or with uptake inhibitors and enhancers. MBO intestinal absorption was compared with an internal standard, mannitol. 35S-MBO demonstrated very little absorption (< 1%) across rat and human intestinal tissues. Transport appeared to be unsaturable up to 500 μM, and relatively insensitive to compounds that opened tight junctions or inhibited P-glycoprotein. However, preliminary studies with Caco-2 cells suggest a possible saturable mechanism at higher ON concentrations. Confocal fluorescence microscopy studies show that fluorescein isothiocyanate (FITC)-MBO was internalized into intestinal cells. Although some differences in ON transport were observed as a function of the transport model, MBO transport was mostly consistent with a transcellular, rather than a paracellular, absorption mechanism. (C) 1999 John Wiley and Sons, Ltd.

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Wu-Pong, S., Livesay, V., Dvorchik, B., & Barr, W. H. (1999). Oligonucleotide transport in rat and human intestine Ussing chamber models. Biopharmaceutics and Drug Disposition, 20(9), 411–416. https://doi.org/10.1002/1099-081X(199912)20:9<411::AID-BDD208>3.0.CO;2-4

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