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首页> 外文期刊>British Journal of Clinical Pharmacology >Intracellular pharmacokinetics of gemcitabine, its deaminated metabolite 2′,2′‐difluorodeoxyuridine and their nucleotides
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Intracellular pharmacokinetics of gemcitabine, its deaminated metabolite 2′,2′‐difluorodeoxyuridine and their nucleotides

机译:吉西他滨的细胞内的药代动力学,其序列化代谢物2',2'-二氟乙基嘌呤及其核苷酸

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Aims Gemcitabine (2′,2′‐difluoro‐2′‐deoxycytidine; dFdC) is a prodrug that has to be phosphorylated within the tumour cell to become active. Intracellularly formed gemcitabine diphosphate (dFdCDP) and triphosphate (dFdCTP) are considered responsible for the antineoplastic effects of gemcitabine. However, a major part of gemcitabine is converted into 2′,2′‐difluoro‐2′‐deoxyuridine (dFdU) by deamination. In the cell, dFdU can also be phosphorylated to its monophosphate (dFdUMP), diphosphate (dFdUDP) and triphosphate (dFdUTP). In vitro data suggest that these dFdU nucleotides might also contribute to the antitumour effects, although little is known about their intracellular pharmacokinetics (PK). Therefore, the objective of the present study was to gain insight into the intracellular PK of all dFdC and dFdU nucleotides formed during gemcitabine treatment. Methods Peripheral blood mononuclear cell (PBMC) samples were collected from 38 patients receiving gemcitabine, at multiple time points after infusion. Gemcitabine, dFdU and their nucleotides were quantified in PBMCs. In addition, gemcitabine and dFdU plasma concentrations were monitored. The individual PK parameters in plasma and in PBMCs were determined. Results Both in plasma and in PBMCs, dFdU was present in higher concentrations than gemcitabine [mean intracellular area under the concentration–time curve from time zero to 24?h (AUC 0–24?h ) 1650 vs. 95?μM*h]. However, the dFdUMP, dFdUDP and dFdUTP concentrations in PBMCs were much lower than the dFdCDP and dFdCTP concentrations. The mean AUC 0–24?h for dFdUTP was 312?μM*h vs. 2640?μM*h for dFdCTP. Conclusions The study provides the first complete picture of all nucleotides that are formed intracellularly during gemcitabine treatment. Low intracellular dFdU nucleotide concentrations were found, which calls into question the relevance of these nucleotides for the cytotoxic effects of gemcitabine.
机译:AIMS GEMCITABINE(2',2'-二氟-2'-脱氧胞苷; DFDC)是必须在肿瘤细胞内磷酸化以变为活性的前药。细胞内形成的吉西他滨二磷酸二磷酸(DFDCDP)和三磷酸(DFDCTP)被认为是吉西他滨的抗肿瘤作用的原因。然而,吉西他滨的主要部分通过脱氧转化为2',2'-二氟-2'-脱氧尿苷(DFDU)。在细胞中,DFDU也可以将其磷酸化到其单磷酸盐(DFdump),二磷酸二磷酸(DFDUDP)和三磷酸(DFDUTP)中。体外数据表明,这些DFDU核苷酸也可能有助于抗肿瘤效果,尽管对其细胞内的药代动力学(PK)知之甚少。因此,本研究的目的是深入了解吉西他滨治疗期间形成的所有DFDC和DFDU核苷酸的细胞内PK。方法在输注后的多个时间点,从接受吉西他滨的38例收集外周血单核细胞(PBMC)样品。吉西他滨,DFDU及其核苷酸在PBMC中量化。此外,监测吉西他滨和DFDU血浆浓度。确定等离子体中的个体PK参数和PBMC。结果血浆和PBMC中的结果,DFDU在比吉西他滨的更高浓度存在[浓度 - 时间曲线下的平均细胞内面积从0到24℃(AUC 0-24ΔH)1650与95.μm* h] 。然而,PBMC中的DFdump,DFDUDP和DFDUTP浓度远低于DFDCDP和DFDCTP浓度。对于DFdutp的平均AUC 0-24?H为DFDCTP的312Ωμm* h与2640.μm* h。结论该研究提供了在吉西他滨治疗期间细胞内形成的所有核苷酸的第一完整图像。发现低细胞内DFDU核苷酸浓度,该核苷酸呼吁质疑这些核苷酸对吉西他滨细胞毒性作用的相关性。

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