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首页> 外文期刊>Drug metabolism and pharmacokinetics. >Biotransformation profiling of ((14)C)ixabepilone in human plasma, urine and feces samples using accelerator mass spectrometry (AMS).
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Biotransformation profiling of ((14)C)ixabepilone in human plasma, urine and feces samples using accelerator mass spectrometry (AMS).

机译:使用加速器质谱(AMS)在人血浆,尿液和粪便中对((14)C)ixabepilone进行生物转化分析。

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摘要

Ixabepilone (BMS-247550, Ixempra is a semi-synthetic analog of the natural product epothilone B and marketed for its use in the treatment of cancer. A conventional human ADME study using decay counting methods for (14)C detection could not be conducted due to the radiolytic instability of [(14)C]ixabepilone at a typical specific activity (generally 1-10 microCi/mg). However, [(14)C]ixabepilone was sufficiently stable at low specific activity (1-2 nCi/mg). These low levels required the use of accelerator mass spectrometry (AMS) for radioactivity detection. The metabolic fate of this compound was investigated in eight patients following single intravenous doses of [(14)C]ixabepilone (70 mg, 80 nCi; specific activity: 1.14 nCi/mg). Metabolite profiles in pooled urine, feces and plasma samples were determined by HPLC-AMS analysis. The major radioactive component in urine and plasma was [(14)C]ixabepilone. Feces had a small amount of ixabepilone. There were numerous other drug-related components in both urine and fecal extracts (each <6% of the administered dose). LC/MS analysis of plasma, urine and feces samples showed the presence of three degradants of ixabepilone and several oxidative metabolites (M+16, M+14 and M-2 metabolites). This study demonstrates the utility of AMS in investigating the metabolite and excretion profiles of [(14)C]ixabepilone following administration to humans.
机译:Ixabepilone(BMS-247550,Ixempra是天然产物埃坡霉素B的半合成类似物,已投放市场用于治疗癌症。由于使用衰变计数方法进行(14)C检测而无法进行常规的人类ADME研究,原因是[(14)C] ixabepilone在典型比活(通常为1-10 microCi / mg)下的辐射不稳定性;但是,[(14C]] ixabepilone在低比活度(1-2 nCi / mg下)足够稳定)。这些低水平需要使用加速器质谱(AMS)进行放射性检测。在单次静脉内注射[(14)C] ixabepilone(70 mg,80 nCi;特异性)后,八名患者研究了该化合物的代谢命运。活性:1.14 nCi / mg)。合并的尿液,粪便和血浆样品中的代谢物谱通过HPLC-AMS分析确定,尿液和血浆中的主要放射性成分为[(14)C] ixabepilone,粪便中含有少量ixabepilone 。还有许多其他与毒品有关的药物尿液和粪便提取物中的成分(均小于给药剂量的6%)。血浆,尿液和粪便样品的LC / MS分析表明,存在伊沙贝比隆的三种降解物和几种氧化代谢物(M + 16,M + 14和M-2代谢物)。这项研究证明了AMS在研究对人给药后[(14)C] ixabepilpilone的代谢物和排泄概况方面的实用性。

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