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Transport and uptake characteristics of a new derivative of berberine (CPU-86017) by human intestinal epithelial cell line: Caco-2

  • China Pharmaceutical University

Research output: Contribution to journalArticlepeer-review

17 Scopus citations

Abstract

AIM: The characteristics of transepithelial transport and uptake of CPU-86017 {[7-(4-chlorbenzyl)-7,8,13,13α-tetrahydroberberine chloride, CTHB]}, a new antiarrhythmia agent and a new derivative of berberine, were investigated on epithelial cell line (Caco-2) to further understand the absorption mechanism of berberine and its derivatives. METHODS: Caco-2 cell was used. RESULTS: 1) The permeability coefficient from the apical (AP) to basolateral (BL) of CPU-86017 was approximately 5 times higher than that from BL-to-AP transport. The effects of a P-glycoprotein (P-gp) inhibitor-cyclosporin A, some surfactants, and lower pH on the transepithelial transport of CPU-86017 were also observed. Cyclosporine A at 7.5 mg/L had no effect on the transepithelial electrical resistance (TEER); an about 4-fold enhancement on the transepithlial transport of CPU-86017 was observed. Some surfactants (sodium citrate, sodium deoxycholate, and sodium dodecyl sulfate) at 100 μmol/L and low pH (pH=6.0) induced a reversible decrease of TEER; enhancements of the transepithelial transport of CPU-86017 were also observed with some surfactants; 2) In the process of uptake of CPU-86017, the initial uptake rates of CPU-86017 were saturable with a Vmax of (250±39) μg·min-1·g-1 (protein) and Km of (0.90±0.12) mmol/L. This process was enhanced by cyclosporine A (7.5 mg/L) with a Vmax of (588±49) μg·min-1·g-1(protein) and Km (0.42±0.08) mmol/L. CONCLUSION: Some surfactants and P-gp inhibitors can be considered as enhancers of its transepithelial transport and uptake.

Original languageEnglish
Pages (from-to)1185-1191
Number of pages7
JournalActa Pharmacologica Sinica
Volume24
Issue number12
StatePublished - Dec 2003
Externally publishedYes

Keywords

  • Berberine
  • CPU-86017
  • Caco-2 cell
  • Cyclosporine A
  • Sodium citrate
  • Sodium deoxycholate
  • Sodium dodecyl sulfate

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