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四氢尿苷联合阿糖胞苷的I期评估

Phase I evaluation of tetrahydrouridine combined with cytosine arabinoside.

作者信息

Wong P P, Currie V E, Mackey R W, Krakoff I H, Tan C T, Burchenal J H, Young C W

出版信息

Cancer Treat Rep. 1979 Aug;63(8):1245-9.

PMID:383291
Abstract

In conventional clinical use, cytosine arabinoside (ara-C) is rapidly deaminated by pyrimidine nucleoside deaminase to the nontoxic compound uracil arabinoside. Tetrahydrouridine (THU) effectively inhibits this enzymatic degradation but is by itself nontoxic. This study demonstrates that concomitant administration of THU markedly increases the myelosuppressive potency of ara-C. When 25 or 50 mg/kg of THU iv and 0.1--0.2 mg/kg of ara-C iv are given daily x 5 days, they produce moderate-to-severe leukopenia and mild-to-moderate thrombocytopenia. A dose of 25 mg/kg of THU with 0.1 mg/kg of ara-C iv daily x 5 days appears appropriate for phase II studies; it produces myelosuppression equivalent to that produced by 3 mg/kg/day x 5 days of ara-C alone. No toxicity occurred with this combination that would not have been expected from ara-C given alone in an equitoxic dose. Although THU and ara-C produced a reduction in peripheral blood and bone marrow blast cells in eight of nine patients with acute leukemia, bone marrow remission did not occur in any of these heavily pretreated patients.

摘要

在传统临床应用中,阿糖胞苷(ara - C)会被嘧啶核苷脱氨酶迅速脱氨,转化为无毒化合物阿糖尿苷。四氢尿苷(THU)能有效抑制这种酶促降解,但其本身无毒。本研究表明,同时给予THU可显著增强ara - C的骨髓抑制效力。当每日静脉注射25或50mg/kg的THU以及0.1 - 0.2mg/kg的ara - C,持续5天时,会产生中度至重度白细胞减少和轻度至中度血小板减少。每日静脉注射25mg/kg的THU与0.1mg/kg的ara - C,持续5天的剂量似乎适用于II期研究;其产生的骨髓抑制作用与单独使用3mg/kg/天×5天的ara - C相当。该联合用药未出现单独给予等毒性剂量ara - C时未预期到的毒性。尽管THU和ara - C使9例急性白血病患者中的8例外周血和骨髓原始细胞减少,但这些经过大量预处理的患者均未出现骨髓缓解。

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