Is there a relationship between cytarabine pharmacokinetics and keratitis?--A case report.

J Boos, T Bömelburg, H Gerding, H Jürgens
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Abstract

While on therapy for acute myeloid leukemia, a 15-year-old girl developed extensive punctate keratitis of both eyes following high-dose cytarabine therapy (HD-Ara-C). Pharmacokinetic monitoring showed an increase of the Ara-C plasma levels up to twice the steady-state level within 10 minutes after discontinuation of the Ara-C infusion. Calculations of Ara-C plasma half-life, plasma clearance and volume of distribution were within the expected range. Owing to the short half-life of Ara-C in blood due to rapid deamination, varying infusion velocities will result in markedly varying plasma levels. Higher peak plasma levels lead to proportionally higher diffusion into compartments like tears, aqueous humor and cerebrospinal fluid. In compartments which lack noteworthy deaminase activity, dose intensity will be much more enhanced than in plasma. Peak plasma levels, therefore, may be associated with multifold local toxicity without concurrent increase of hematological toxicity. Especially when the drug is given in small volumes of infusion, these considerations should be taken into account. Precise control of infusion parameters and application of artificial tears for dilution of the Ara-C concentration on the corneal surface should be part of keratitis prophylaxis.

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阿糖胞苷药代动力学与角膜炎有关系吗?——病例报告。
在接受急性髓性白血病治疗期间,一名15岁女孩在接受高剂量阿糖胞苷治疗(HD-Ara-C)后出现双眼广泛的点状角膜炎。药代动力学监测显示,停用阿拉c后10分钟内,血浆中阿拉c水平升高至稳态水平的两倍。Ara-C等离子体半衰期、等离子体清除率和分布体积的计算均在预期范围内。由于Ara-C在血液中的半衰期短,脱氨快,不同的输注速度会导致血浆水平的显著变化。较高的峰值血浆水平导致成比例的更高的扩散到诸如泪液、房水和脑脊液等腔室。在缺乏明显脱氨酶活性的腔室中,剂量强度将比血浆中增强得多。因此,血药浓度峰值可能与多重局部毒性有关,但不会同时增加血液毒性。特别是当药物以小体积输注时,应考虑到这些因素。准确控制输液参数和应用人工泪液稀释角膜表面的Ara-C浓度应成为预防角膜炎的一部分。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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