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Effects of Piperazine Derivative on Paclitaxel Pharmacokinetics

机译:哌嗪衍生物对紫杉醇药代动力学的影响

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摘要

Paclitaxel (PTX) is an anticancer agent that is used to treat many cancers but it has a very low oral bioavailability due, at least in part, to the drug efflux transporter, P-glycoprotein (P-gp). Therefore, this study was performed to enhance oral bioavailability of PTX. In this study, we investigated the effects of several piperazine derivatives on P-gp function in vitro. Compound >4 was selected as the most potent P-gp inhibitor from the in vitro results for examining the pharmacokinetic (PK) changes of PTX in rats. Compound 4 increased the AUCinf of PTX without alterations in the Cmax value. The elimination half-life was extended and the oral clearance decreased. Additionally, the Tmax was delayed or widened in the treatment groups. Therefore, the bioavailability (BA) of PTX was improved 2.1-fold following the co-administration of 5 mg/kg of the derivative. A piperazine derivative, compound 4, which was confirmed as a substantial P-gp inhibitor in vitro increased the BA of PTX up to 2-fold by a lingering absorption, in part due to inhibition of intestinal P-gp and a low oral clearance of PTX. These results suggest that co-administering compound >4 may change the PK profile of PTX by inhibiting P-gp activity in the body.
机译:紫杉醇(PTX)是一种抗癌药,用于治疗许多癌症,但至少部分归因于药物外排转运蛋白P-糖蛋白(P-gp),口服生物利用度非常低。因此,进行该研究以增强PTX的口服生物利用度。在这项研究中,我们调查了几种哌嗪衍生物对体外P-gp功能的影响。从体外结果中选择化合物> 4 作为最有效的P-gp抑制剂,以检查PTX在大鼠中的药代动力学(PK)变化。化合物4增加了PTX的AUCinf,而没有改变Cmax值。消除半衰期延长,口腔清除率降低。另外,在治疗组中,Tmax被延迟或加宽。因此,在并用5 mg / kg衍生物后,PTX的生物利用度(BA)提高了2.1倍。哌嗪衍生物化合物4在体外被证实是一种重要的P-gp抑制剂,其持久吸收使PTX的BA升高至2倍,部分原因是抑制了肠道P-gp和低的口服清除率。 PTX。这些结果表明,共同给药化合物> 4 可能会通过抑制体内P-gp活性来改变PTX的PK分布。

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