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继发性白血病:挑战与研究方向

The secondary leukemias: challenges and research directions.

作者信息

Smith M A, McCaffrey R P, Karp J E

机构信息

National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

J Natl Cancer Inst. 1996 Apr 3;88(7):407-18. doi: 10.1093/jnci/88.7.407.

Abstract

Acute myelogenous leukemia (AML) arising following exposure to genotoxic agents has been recognized as a distinctive entity for more than 40 years. Secondary, or therapy-related, AML accounts for 10%-20% of all AML cases. This review addresses four overarching areas of investigation focused on secondary AMLs: 1) dissection of the molecular structure of the induced genetic lesions and identification of the functional consequences of these changes, thereby providing clues to the pathogenesis of secondary AML and potentially serving as a basis for innovative therapeutic interventions; 2) identification and characterization of mechanisms of DNA damage and the orderly repair of such damage; 3) identification and application of accurate biomarkers of leukemogenesis for the purpose of risk prediction and quantification, potentially allowing recognition of patients especially susceptible to the leukemogenic effects of chemotherapy (for genetic or acquired reasons) and allowing their treatment for cancer to be modified on the basis of this susceptibility; and 4) design and implementation of longitudinal clinical and genetic monitoring of high-risk populations (i.e., individuals under-going cytotoxic therapies for primary cancers). This review of the literature relating to these areas builds upon these themes and attempts to synthesize these seemingly disparate areas of research so that they can be more effectively utilized together to address the problem of secondary AML. Ultimately, the evaluation of these areas will improve our understanding of de novo leukemia and will serve as a springboard for the development of new concepts of therapy and prevention.

摘要

接触基因毒性剂后发生的急性髓系白血病(AML)在40多年前就已被确认为一种独特的疾病实体。继发性或治疗相关的AML占所有AML病例的10%-20%。本综述涉及针对继发性AML的四个总体研究领域:1)剖析诱导的基因损伤的分子结构并确定这些变化的功能后果,从而为继发性AML的发病机制提供线索,并有可能作为创新治疗干预措施的基础;2)鉴定和表征DNA损伤机制以及此类损伤的有序修复;3)鉴定和应用白血病发生的准确生物标志物以进行风险预测和量化,这有可能识别出(因遗传或后天原因)特别易受化疗致白血病作用影响的患者,并根据这种易感性调整其癌症治疗方案;4)设计和实施对高危人群(即正在接受原发性癌症细胞毒性治疗的个体)的纵向临床和基因监测。本对与这些领域相关的文献的综述基于这些主题,并试图综合这些看似不同的研究领域,以便它们能够更有效地共同用于解决继发性AML问题。最终,对这些领域的评估将增进我们对原发性白血病的理解,并将成为开发新治疗和预防概念的跳板。

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