首页> 外文期刊>The Journal of Clinical Pharmacology: Official Journal of the American College of Clinical Pharmacology >Integrating Dynamic Positron Emission Tomography and Conventional Pharmacokinetic Studies to Delineate Plasma and Tumor Pharmacokinetics of FAU, a Prodrug Bioactivated by Thymidylate Synthase
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Integrating Dynamic Positron Emission Tomography and Conventional Pharmacokinetic Studies to Delineate Plasma and Tumor Pharmacokinetics of FAU, a Prodrug Bioactivated by Thymidylate Synthase

机译:将动态正电子发射断层扫描和常规药代动力学研究整合到替代血浆和肿瘤药代动力学,由胸苷合酶生物激活的前药

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摘要

FAU, a pyrimidine nucleotide analogue, is a prodrug bioactivated by intracellular thymidylate synthase to form FMAU, which is incorporated into DNA, causing cell death. This study presents a model-based approach to integrating dynamic positron emission tomography (PET) and conventional plasma pharmacokinetic studies to characterize the plasma and tissue pharmacokinetics of FAU and FMAU. Twelve cancer patients were enrolled into a phase 1 study, where conventional plasma pharmacokinetic evaluation of therapeutic FAU (50-1600 mg/m(2)) and dynamic PET assessment of F-18-FAU were performed. A parent-metabolite population pharmacokinetic model was developed to simultaneously fit PET-derived tissue data and conventional plasma pharmacokinetic data. The developed model enabled separation of PET-derived total tissue concentrations into the parent drug and metabolite components. The model provides quantitative, mechanistic insights into the bioactivation of FAU and retention of FMAU in normal and tumor tissues and has potential utility to predict tumor responsiveness to FAU treatment.
机译:FAU,嘧啶核苷酸类似物是通过细胞内胸苷合酶的前药,以形成FMAU,其掺入DNA中,导致细胞死亡。该研究提出了一种基于模型的方法,用于整合动态正电子发射断层扫描(PET)和常规血浆药代动力学研究,以表征FAU和FMAU的血浆和组织药代动力学。 12名癌症患者注册到1期研究中,其中进行治疗性的常规血浆药代动力学评估(50-1600mg / m(2))和F-18-FAU的动感宠物评估。开发了亲本质代谢物群体药代动力学模型以同时适应宠物衍生的组织数据和常规血浆药代动力学数据。开发模型使PET衍生的总组织浓度的分离进入母体药物和代谢物组分中。该模型提供了对FAU生物活化的定量,机械洞察,并在正常和肿瘤组织中保留FMAU,并具有预测对FAU处理的肿瘤反应性的潜在效用。

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