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首页> 外文期刊>Chemical research in toxicology >Identification of the Novel Capecitabine Metabolites in Capecitabine-Treated Patients with Hand-Foot Syndrome
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Identification of the Novel Capecitabine Metabolites in Capecitabine-Treated Patients with Hand-Foot Syndrome

机译:鉴定Capecitabine治疗的手足综合征患者的新型Capecitabine代谢物

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摘要

Hand-foot syndrome (HFS), the most common side effect of capecitabine, is a dose-limiting cutaneous toxicity with only rare therapeutic options. The causative mechanisms of HFS are still unclear. Many studies suggested that capecitabine or its metabolites caused the toxicity. This study is attempting to determine if there are any new metabolites that may be present and be linked to toxicity. For this purpose, 25 patients who ingested capecitabine orally were enrolled and divided into HFS positive and negative groups. Urine and plasma samples were collected before administration and five cycles after administration. Eleven phase I and phase II metabolites of capecitabine were detected and identified by ultraperformance liquid chromatography coupled with quadrupole time-of-flight tandem mass spectrometry with a metabolomic approach and MetaboLynx(XS). Nine novel metabolites of capecitabine were identified herein, which were not observed in the HFS negative group. Their structures were confirmed by chemical synthesis and nuclear magnetic resonance spectroscopy. The cytotoxities of capecitabine and its metabolites on HaCaT cells were measured. Among them, M9/10 exhibited significant inhibitory activity, and they were produced via acetylation mainly by N-acetyltransferase 2. Our study comprehensively described the metabolism of capecitabine in patients with HFS and detected the novel pathways of capecitabine, which was a positive significance for the mechanism of HFS.
机译:手足综合征(HFS),葡萄球菌列明的最常见的副作用是一种剂量限制皮肤毒性,只有罕见的治疗选择。 HFS的致病机制尚不清楚。许多研究表明Capecitabine或其代谢物导致毒性。该研究试图确定是否存在任何可能存在的新代谢物并与毒性相关。为此目的,将25名摄入杂志的患者口服,并分为HFS阳性和阴性群体。在给药之前收集尿液和血浆样品,并在给药后进行5个循环。通过超大液相色谱法检测并鉴定与四极其飞行时间串联质谱和代谢物方法和代谢单词(Xs)的超细液相色谱法检测并鉴定了亚二元素的11相二代谢物。本文鉴定了九种新代谢石的新代谢物,在HFS阴性组中未观察到。通过化学合成和核磁共振光谱证实了它们的结构。测定了Capecitabine的细胞毒性及其在HaCAT细胞上的代谢物。其中,M9 / 10表现出显着的抑制活性,它们主要由乙酰化产生,主要由N-乙酰转移酶2制备。我们的研究全面地描述了HFS患者的Capecitabine的代谢,并检测了Capecitabine的新途径,这是一种积极意义HFS的机制。

著录项

  • 来源
    《Chemical research in toxicology》 |2018年第10期|共11页
  • 作者单位

    Zhejiang Univ Collaborat Innovat Ctr Diag &

    Treatment Infect Di State Key Lab Diag &

    Treatment;

    Zhejiang Univ Collaborat Innovat Ctr Diag &

    Treatment Infect Di State Key Lab Diag &

    Treatment;

    Zhejiang Inst Food &

    Drug Control Hangzhou 310004 Zhejiang Peoples R China;

    PLA Hosp 117 Dept Oncol 14 Lingyin Rd Hangzhou 310013 Zhejiang Peoples R China;

    Zhejiang Univ Collaborat Innovat Ctr Diag &

    Treatment Infect Di State Key Lab Diag &

    Treatment;

    Zhejiang Univ Collaborat Innovat Ctr Diag &

    Treatment Infect Di State Key Lab Diag &

    Treatment;

    Zhejiang Univ Collaborat Innovat Ctr Diag &

    Treatment Infect Di State Key Lab Diag &

    Treatment;

    Zhejiang Univ Collaborat Innovat Ctr Diag &

    Treatment Infect Di State Key Lab Diag &

    Treatment;

    Zhejiang Univ Lab Pharmaceut Anal &

    Drug Metab Zhejiang Prov Key Lab Anticanc Drug Res Coll;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 毒物学(毒理学);
  • 关键词

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