AI Article Synopsis

  • Coadministration of certain enteral nutrients (ENs) negatively impact the absorption of the antiepileptic drug phenytoin (PHT), but the underlying mechanisms remain unclear.
  • Researchers used a model with Caco-2 cells to investigate how different nutrients affect the permeability of PHT, finding that casein, digested soy protein, and dextrin significantly reduced its absorption, while digested casein had the opposite effect.
  • The study concludes that the composition of ENs can influence PHT absorption, which is crucial for determining the best ENs to use alongside oral PHT treatment.

Article Abstract

Background: Previously, we revealed that coadministration of particular enteral nutrients (ENs) decreases plasma concentrations and gastric absorption of phenytoin (PHT), an antiepileptic drug, in rats; however, the mechanism has not been clarified.

Methods: We measured the permeability rate of PHT using a Caco-2 cell monolayer as a human intestinal absorption model with casein, soy protein, simulated gastrointestinal digested casein protein (G-casein or P-casein) or simulated gastrointestinal digested soy protein (G-soy or P-soy), dextrin, sucrose, degraded guar gum, indigestible dextrin, calcium, and magnesium, which are abundant in the ENs, and measured the solution's properties.

Results: We demonstrated that casein (40 mg/ml), G-soy or P-soy (10 mg/ml), and dextrin (100 mg/ml) significantly decreased the permeability rate of PHT compared with the control. By contrast, G-casein or P-casein significantly increased the permeability rate of PHT. We also found that the PHT binding rate to casein 40 mg/ml was 90%. Furthermore, casein 40 mg/ml and dextrin 100 mg/ml have high viscosity. Moreover, G-casein and P-casein significantly decreased the transepithelial electrical resistance of Caco-2 cell monolayers compared with casein and the control.

Conclusion: Casein, digested soy protein, and dextrin decreased the gastric absorption of PHT. However, digested casein decreased PHT absorption by reducing the strength of tight junctions. The composition of ENs may affect the absorption of PHT differently, and these findings would aid in the selection of ENs for orally administered PHT.

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Source
http://dx.doi.org/10.1002/jpen.2542DOI Listing

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