Purpose: To evaluate the pharmacokinetics of the major compounds in Ginkgo leaf dosage formulations (namely, Yikangning tablets, Ginaton tablets, Aoshi dropping pills and Yinxinke dispersible tablets), commonly used in traditional Chinese medicine.
Methods: A randomized 4*4 crossover study with eight beagle dogs was carried out. Plasma samples were collected following oral administration of four different preparations and the effective ingredients, namely, kaempferol, quercetin, isorhamnetin, ginkgolides A, ginkgolides B, ginkgolides C and bilobalide were detected by a validated ultra-performance liquid chromatography-tandem mass spectrometry (UPLC-TMS). Then the pharmacokinetics of these target compounds, of  different preparations were studied.
Results: The adjusted pharmacokinetic data showed that the area under the concentration-time curve from time-zero to the last measurable concentration  (AUC0-t) of kaempferol, quercetin, isorhamnetin, bilobalide, ginkgolides A, ginkgolides B, and ginkgolides C in plasma ranged from 124.37 ± 90.46 to 2261.87 ±  812.35, after administration of Yikangning; 142.28 ± 62.37 to 2529.46 ± 320.48 μg/L•h following administration of Ginaton; 158.52 ± 55.48 to 1987.40 ± 766.21  μg/L•h after Aoshi administration; 160.49 ± 104.66 to 2016.92 ± 1150.92 μg/L•h following Yinxinke administration. The results also indicate that the flavonoids  (especially quercetin) in dispersible tablets and dropping pills hexhibited higher AUC than those in conventional tablets. There were no differences between Aoshi (dropping pills) and Yinxinke (dispersible tablets) in terms of the bioavailability of the flavonoids, but the dropping pill flavonoids showed lower tmax.
Conclusion: The results indicate that UPLC-TMS can used to simultaneously evaluate the plasma pharmacokinetics of Ginko compounds in beagle dogs

Keywords: Ginkgo biloba, Beagle dog plasma, Kaempferol, Quercetin, Isorhamnetin, Ginkgolides A, Ginkgolides B, Ginkgolides C, Bilobalide, Pharmacokinetics; Bioavailability