Frontiers in Pharmacology (May 2019)

A Single Dose of Baicalin Has No Clinically Significant Effect on the Pharmacokinetics of Cyclosporine A in Healthy Chinese Volunteers

  • Ruijuan Liu,
  • Ruijuan Liu,
  • Xia Li,
  • Jingyao Wei,
  • Jingyao Wei,
  • Shuaibing Liu,
  • Shuaibing Liu,
  • Yuanyuan Chang,
  • Yuanyuan Chang,
  • Jiali Zhang,
  • Jiali Zhang,
  • Ji Zhang,
  • Ji Zhang,
  • Xiaojian Zhang,
  • Xiaojian Zhang,
  • Uwe Fuhr,
  • Max Taubert,
  • Xin Tian,
  • Xin Tian

DOI
https://doi.org/10.3389/fphar.2019.00518
Journal volume & issue
Vol. 10

Abstract

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Despite its narrow therapeutic window and large interindividual variability, cyclosporine A (CsA) is the first-line therapy following organ transplantation. Metabolized mainly by CYP3A and being a substrate of P-glycoprotein (P-gp), CsA is susceptible to drug–drug interactions. Baicalin (BG) is a drug used for adjuvant therapy of hepatitis in traditional Chinese medicine. Since its aglycone baicalein (B) inhibits CYP3A and P-gP, co-administration might affect CsA pharmacokinetics. This study investigated the effect of BG on CsA pharmacokinetics. In a two-period study, 16 healthy volunteers received a single 200 mg oral CsA dose alone (reference period) or in combination with 500 mg BG (test period). Pharmacokinetic evaluation of CsA was carried out using non-compartmental analysis (NCA) and population pharmacokinetics (popPK). Treatments were compared using the standard bioequivalence method. Based on NCA, 90% CIs of AUC and Cmax test-to-reference ratios were within bioequivalence boundaries. In the popPK analysis, a two-compartment model (clearance/F 62.8 L/h, central and peripheral volume of distribution/F 254 L and 388 L) with transit compartments for absorption appropriately described CsA concentrations. No clinically relevant effect of 500 mg BG co-administration on CsA pharmacokinetics was identified and both treatments were well tolerated.

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