Table 3.
Summary of studies investigating the effect of chitosan and its derivatives on the intestinal permeability and oral pharmacokinetic parameters of drugs.
| Drug (s) | Absorption Enhancer | Model | Results | Ref. |
|---|---|---|---|---|
| Acyclovir | Chitosan | In vitro: Caco-2 cell | Papp: 124- and 143-fold increase | [83] |
| In vivo: rat intestine | AUC0–12 and AUC0–∞: 0.70- and 0.74-fold decrease Cmax: 0.56- and 0.63-fold decrease Tmax: 1.25- and 1.50-fold increase |
|||
| In vitro: Ussing chamber | Papp: 1.08- and 2.33-fold increase | |||
| Glucosamine hydrochloride | Chitosan | In vitro: Caco-2 cell | Papp: 1.9, 2.5 and 4.0-fold increase | [88] |
| In vivo: rat intestine | Cmax: 2.8-fold increase Tmax: no change AUC0−∞: 2.5-fold increase |
|||
| Salvianolic acid B | Chitosan | In vitro: Caco-2 cell | Papp: 4.43-fold increase | [79] |
| In vivo: rat intestine | AUC0–∞: 4.25-fold increase | |||
| Berberine | Chitosan hydrochloride | In vivo: rat intestine | AUC0–36: no improvement Cmax: no improvement |
[86] |
| Chitosan | In vivo: rat intestine | AUC0–36: maximum 2.5-fold increase | ||
| Amphotericin B | Trimethyl chitosan | In vitro: Caco-2 cell | Papp: 1.11-fold increase | [87] |