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对接受急性淋巴细胞白血病治疗的儿童红细胞内氨基蝶呤多聚谷氨酸进行高效液相色谱分离。

High-performance liquid chromatography separation of aminopterin-polyglutamates within red blood cells of children treated for acute lymphoblastic leukemia.

作者信息

Vijayanathan Veena, Smith Angela K, Zebala John A, Kamen Barton A, Cole Peter D

机构信息

Pediatric Hematology/Oncology, The Cancer Institute of New Jersey, Robert Wood Johnson Medical School/UMDNJ, New Brunswick, NJ, USA.

出版信息

Transl Res. 2007 Dec;150(6):367-73. doi: 10.1016/j.trsl.2007.08.002. Epub 2007 Sep 7.

Abstract

Aminopterin (AMT), like the related compound methotrexate (MTX), is a drug with anticancer and antiinflammatory efficacy that works by interfering with synthetic reactions dependent on the vitamin folic acid. Red blood cell (RBC) precursors will accumulate antifolates like AMT and MTX through the same mechanism by which they take up folate. Intracellular folate and antifolates are then metabolized to polyglutamates that remain within the mature RBCs. RBC MTX has been correlated with toxicity and/or treatment efficacy among patients with acute lymphoblastic leukemia (ALL) or rheumatoid arthritis. Because AMT may offer clinically relevant advantages over MTX, we are testing whether it can be administered safely in multiagent therapy to children with ALL. Total RBC AMT was measured to monitor compliance with this oral, outpatient regimen, and to estimate AMT exposure to the bone marrow. Here we describe methods for quantifying each AMT-polyglutamate species within the RBCs of patients. The assay was linear over a concentration range of 62.5-500 nmol/L. Recovery of individual AMT-polyglutamates ranged from 85% to 92%, and the intraday coefficients of variation were 1.3% to 3.6%. Long-chain AMT-polyglutamates (triglutamate and tetraglutamate forms) accounted for over 40% of intracellular AMT within the RBCs of patients. Patients with long-chain AMT polyglutamate concentrations above the median tended to have lower mean neutrophil counts during weekly AMT therapy, which suggests that RBC AMT polyglutamate accumulation may correlate with hematologic toxicity. As AMT continues to be tested in clinical trials, the methods described here will be useful to define relationships between clinical response to AMT and RBC accumulation of AMT-polyglutamates.

摘要

氨蝶呤(AMT)与相关化合物甲氨蝶呤(MTX)一样,是一种具有抗癌和抗炎功效的药物,其作用机制是干扰依赖维生素叶酸的合成反应。红细胞(RBC)前体通过摄取叶酸的相同机制积累AMT和MTX等抗叶酸药物。细胞内的叶酸和抗叶酸药物随后被代谢为多聚谷氨酸,这些多聚谷氨酸会保留在成熟的红细胞内。在急性淋巴细胞白血病(ALL)或类风湿关节炎患者中,红细胞MTX与毒性和/或治疗效果相关。由于AMT可能比MTX具有临床相关优势,我们正在测试它是否能在多药联合治疗中安全地用于ALL儿童。测量红细胞总AMT以监测对这种口服门诊治疗方案的依从性,并估计AMT对骨髓的暴露量。在这里,我们描述了定量患者红细胞内每种AMT - 多聚谷氨酸物种的方法。该测定在62.5 - 500 nmol/L的浓度范围内呈线性。单个AMT - 多聚谷氨酸的回收率在85%至92%之间,日内变异系数为1.3%至3.6%。长链AMT - 多聚谷氨酸(三谷氨酸和四谷氨酸形式)占患者红细胞内细胞内AMT的40%以上。在每周AMT治疗期间,长链AMT多聚谷氨酸浓度高于中位数的患者往往平均中性粒细胞计数较低,这表明红细胞AMT多聚谷氨酸的积累可能与血液学毒性相关。随着AMT在临床试验中继续接受测试,这里描述的方法将有助于确定AMT的临床反应与AMT - 多聚谷氨酸在红细胞中的积累之间的关系。

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