Phase I evaluation of crisnatol (BWA770U mesylate) on a monthly extended infusion schedule.

P W Cobb, K A Havlin, J G Kuhn, J B Craig, G S Harman, J S Luther, J N Turner, G R Weiss, D A Tweedy, J Koeller
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引用次数: 2

Abstract

Crisnatol is an arylmethylaminopropanediol derivative that has shown promise as an antitumor agent in preclinical testing. In a phase I trial using a monthly six-hour infusion schedule the recommended dose for future phase II trials was found to be 388 mg/m2. Neurologic toxicity was dose-limiting in that trial and correlated with the attainment of a threshold plasma concentration of greater than 4.5 micrograms/ml. In this study we treated 15 patients with escalating doses of crisnatol from 450 mg/m2 to 900 mg/m2 administered at a rate of 50 mg/m2/hr over 9, 12, 15, and 18 hours. Toxicity was mild to moderate at all dose levels. However, serious central nervous system effects were noted in one patient at 900 mg/m2 over 18 hours whose plasma level was 6.5 micrograms/ml. This study has demonstrated higher total doses of crisnatol can be given if the drug is administered as a prolonged infusion in an attempt to avoid high plasma levels of the agent.

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crisnatol (BWA770U甲磺酸)每月延长输注计划的I期评估。
Crisnatol是一种芳基甲基氨基丙二醇衍生物,在临床前测试中显示出作为抗肿瘤药物的前景。在使用每月6小时输注计划的I期试验中,发现未来II期试验的推荐剂量为388 mg/m2。在该试验中,神经毒性是剂量限制性的,与达到大于4.5微克/毫升的阈值血浆浓度相关。在这项研究中,我们治疗了15名患者,以50mg /m2/小时的速度递增crisnatol的剂量,从450mg /m2增加到900mg /m2,持续9、12、15和18小时。在所有剂量水平下,毒性均为轻度至中度。然而,一名患者在服用900 mg/m2超过18小时后,其血浆水平为6.5微克/毫升,出现了严重的中枢神经系统影响。这项研究表明,如果长期输注药物以避免高血浆水平的药物,则可以给予更高的crisnatol总剂量。
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