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我们应如何最佳监测 5-FU 的给药以实现效益风险比最大化?

How can we best monitor 5-FU administration to maximize benefit to risk ratio?

机构信息

a Centre Hospitalo-Universitaire de Dijon-Bourgogne , Dijon , France.

b Service de Pharmacologie Clinique , Laboratoire de Pharmacologie Expérimentale et Clinique, Centre d'Investigation Clinique INSERM 1414, CHU de Rennes, Université Rennes 1 , Rennes , France.

出版信息

Expert Opin Drug Metab Toxicol. 2018 Dec;14(12):1303-1313. doi: 10.1080/17425255.2018.1550484. Epub 2018 Nov 23.

Abstract

5-Fluorouracil (5-FU) is currently used as a chemotherapy in several cancers such as head-and-neck (H&N) and colorectal cancers. 5-FU dosing is traditionally based on body surface area (BSA), but this strategy is usually associated with severe toxicities. 5-FU is mainly catabolized by dihydropyrimidine dehydrogenase (DPD), and 5-FU dosage adaptation according to DPD status at the first cycle of treatment is now recommended. To further optimize 5-FU-based chemotherapy, a body of evidences justifies therapeutic drug monitoring (TDM). Areas covered: 5-FU pharmacokinetics, relationships between pharmacokinetics and efficacy or toxicity of 5-FU, proofs of interest of 5-FU TDM and its practical considerations are discussed. Expert opinion: BSA-adjusted 5-FU administration is associated with a large inter-individual variability, and according to this strategy, many patients experience under- or overexposure. Moreover, relationships between 5-FU area under the curve (AUC) and its toxicity or efficacy have been demonstrated, at least in patients with colorectal or H&N cancers. 5-FU therapeutic index has been validated and algorithms of 5-FU dosage adaptation according to its AUC are now available. Advances in pre-analytical and analytical steps of 5-FU TDM make its use feasible in clinical practice. Thus, there are consistent evidences to recommend 5-FU TDM in patients with advanced colorectal or H&N cancers.

摘要

5-氟尿嘧啶(5-FU)目前被用于多种癌症的化疗,如头颈部(H&N)和结直肠癌。5-FU 的剂量传统上基于体表面积(BSA),但这种策略通常与严重的毒性有关。5-FU 主要由二氢嘧啶脱氢酶(DPD)代谢,目前建议在治疗的第一个周期根据 DPD 状态调整 5-FU 剂量。为了进一步优化基于 5-FU 的化疗,大量证据支持治疗药物监测(TDM)。涵盖领域:5-FU 药代动力学、5-FU 药代动力学与疗效或毒性之间的关系、5-FU TDM 的应用证据及其实际考虑因素进行了讨论。专家意见:BSA 调整的 5-FU 给药与个体间的巨大差异有关,根据这种策略,许多患者经历了剂量不足或过量。此外,已经证明了 5-FU 曲线下面积(AUC)与其毒性或疗效之间的关系,至少在结直肠癌或 H&N 癌症患者中是如此。5-FU 治疗指数已得到验证,现在可根据 AUC 调整 5-FU 剂量的算法。5-FU TDM 的分析前和分析步骤的进展使得其在临床实践中具有可行性。因此,有充分的证据建议在晚期结直肠癌或 H&N 癌症患者中进行 5-FU TDM。

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