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氨苯砜:治疗耐药和继发性急性髓细胞白血病的未来?

Amonafide: a future in treatment of resistant and secondary acute myeloid leukemia?

机构信息

Mayo Clinic Phoenix Campus, Department of Hematology & Oncology, 5777 East Mayo Boulevard, Phoenix, AZ 85054, USA.

出版信息

Expert Rev Hematol. 2012 Feb;5(1):17-26. doi: 10.1586/ehm.11.68.

Abstract

Development of the novel topoisomerase II inhibitor, amonafide, began almost 40 years ago. The drug was selected for further investigation owing to evidence of marked antineoplastic efficacy in preclinical models of cancer. When its usefulness in the treatment of various solid malignancies proved limited, focus was shifted to establishing its use as an antileukemic agent, specifically against secondary and treatment-associated acute myeloid leukemia (AML). While Phase I and II studies gave rise to hopes that amonafide might hold the key to treating older patients, including those with multidrug resistant, cytogenetically unfavorable secondary and treatment-associated AML, when used in combination with cytarabine, it failed to demonstrate a survival advantage over standard-of-care therapy in randomized studies. This article will outline the development of amonafide from the laboratory to the bedside and discuss the potential place that this agent has in the current management of AML.

摘要

新型拓扑异构酶 II 抑制剂氨萘非特的研发工作始于近 40 年前。该药物因其在癌症临床前模型中具有显著抗肿瘤功效的证据而被选中进行进一步研究。当它在治疗各种实体恶性肿瘤方面的用途被证明有限时,研究重点转向将其用作抗白血病药物,特别是针对继发性和治疗相关的急性髓细胞性白血病(AML)。虽然 I 期和 II 期研究让人们有希望认为氨萘非特可能是治疗老年患者的关键,包括那些对多药耐药、细胞遗传学不利的继发性和治疗相关的 AML 患者,但当与阿糖胞苷联合使用时,它未能在随机研究中显示出比标准治疗更优的生存优势。本文将概述氨萘非特从实验室到临床的发展历程,并讨论该药物在 AML 目前治疗中的潜在地位。

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