Publications by authors named "Aoi Yoshitomo"

Drug absorption from the gastrointestinal tract is often restricted by efflux transport by P-glycoprotein (P-gp) and metabolism by CYP3A4. Both localize in the epithelial cells, and thus, their activities are directly affected by the intracellular drug concentration, which should be regulated by the ratio of permeability between apical (A) and basal (B) membranes. In this study, using Caco-2 cells with forced expression of CYP3A4, we assessed the transcellular permeation of A-to-B and B-to-A directions and the efflux from the preloaded cells to both sides of 12 representative P-gp or CYP3A4 substrate drugs and obtained the parameters for permeabilities, transport, metabolism, and unbound fraction in the enterocytes (f) using simultaneous and dynamic model analysis.

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Article Synopsis
  • A study evaluated how eight cytochrome P450 (CYP) isoenzymes inhibit various substances, including pesticides, to assess the risks of drug interactions (DIs), especially with CYPs.
  • Voriconazole, an azole antifungal, was found to significantly inhibit CYP2B6, affecting cyclophosphamide's metabolism and reducing its adverse effects in mice by about 50%.
  • Analysis of adverse event databases revealed that combining cyclophosphamide and azoles like voriconazole mostly led to reduced instances of neutropenia, hemorrhagic cystitis, and alopecia, suggesting that CYP2B6-mediated drug interactions need closer examination in clinical practice.
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Precise prediction of drug absorption is key to the success of new drug development and efficacious pharmacotherapy. In this study, we developed a new absorption model, the advanced translocation model (ATOM), by extending our previous model, the translocation model. ATOM reproduces the translocation of a substance in the intestinal lumen using a partial differential equation with variable dispersion and convection terms to describe natural flow and micromixing within the intestine under not only fasted but also fed conditions.

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