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Mar Drugs
2016 Jun 17;146:. doi: 10.3390/md14060114.
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Absorption and Transport of Sea Cucumber Saponins from Apostichopus japonicus.
Li S
,
Wang Y
,
Jiang T
,
Wang H
,
Yang S
,
Lv Z
.
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The present study is focused on the intestinal absorption of sea cucumber saponins. We determined the pharmacokinetic characteristics and bioavailability of Echinoside A and Holotoxin A₁; the findings indicated that the bioavailability of Holotoxin A₁ was lower than Echinoside A. We inferred that the differences in chemical structure between compounds was a factor that explained their different characteristics of transport across the intestine. In order to confirm the absorption characteristics of Echinoside A and Holotoxin A₁, we examined their transport across Caco-2 cell monolayer and effective permeability by single-pass intestinal perfusion. The results of Caco-2 cell model indicate that Echinoside A is transported by passive diffusion, and not influenced by the exocytosis of P-glycoprotein (P-gp, expressed in the apical side of Caco-2 monolayers as the classic inhibitor). The intestinal perfusion also demonstrated well the absorption of Echinoside A and poor absorption of Holotoxin A₁, which matched up with the result of the Caco-2 cell model. The results demonstrated our conjecture and provides fundamental information on the relationship between the chemical structure of these sea cucumber saponins and their absorption characteristics, and we believe that our findings build a foundation for the further metabolism study of sea cucumber saponins and contribute to the further clinical research of saponins.
Figure 1. ESI-MS spectra of Echinoside A in negative mode.
Figure 2. Chemical structure of Holotoxin A1.
Figure 3. Chemical structure of Echinoside A.
Figure 4. HPLC-chromatogram of Echinoside A and Holotoxin A1.
Figure 5. (a) Plasma concentrations-time curves of Echinoside A after oral administration; (b) plasma concentrations-time curves of Echinoside A after intravenous administration; and (c) plasma concentrations-time curves of Holotoxin A1 after intravenous administration. (means ± SD, n = 5).
Figure 6. (a) AP-to-BL transport of different concentration of Echinoside A across Caco-2 monolayers; and (b) BL-to-AP transport of different concentration of Echinoside A across Caco-2 monolayers, (means ± SD, n = 3).
Figure 8. Peff values of Echinoside A and Holotoxin A1 at 1, 5, 25 μg/mL, as well as 50 μg/mL with the addition of verapamil using single-pass intestinal perfusion (means ± SD, n = 5).
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