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三氧化二砷作为急性早幼粒细胞白血病的一线治疗药物。

Arsenic trioxide as first-line treatment for acute promyelocytic leukemia.

机构信息

Department of Pharmacy, Inova Fairfax Hospital, Falls Church, VA, USA.

出版信息

Am J Health Syst Pharm. 2009 Nov 1;66(21):1913-8. doi: 10.2146/ajhp080342.

DOI:10.2146/ajhp080342
PMID:19850784
Abstract

PURPOSE

The history, clinical pharmacology and toxicities, and role of arsenic trioxide as a first-line agent for treating acute promyelocytic leukemia (APL) are described.

SUMMARY

APL is most often characterized by the hallmark reciprocal translocation between chromosomes 15 and 17, leading to the fusion of the promyelocytic gene and retinoic acid receptor alpha. Arsenic's therapeutic utility as an antileukemic agent was first described in the late 18th century. Arsenic trioxide demonstrates a dual, dose-dependent mechanism of action and can induce both partial myeloid differentiation and apoptosis. Arsenic trioxide is generally well tolerated, with reversible toxicities rarely requiring discontinuation of therapy. Toxicities associated with arsenic trioxide include leukocytosis, Q-T interval prolongation, APL differentiation syndrome, and hepatotoxicity. Since 2000, arsenic trioxide has been used as the standard of care for relapsed APL, with remission rates greater than 80% as a single agent. In an attempt to maximize disease-free survival and minimize relapse rates in patients with APL, arsenic trioxide is now being investigated as first-line therapy in the management of APL, with several studies showing promising outcomes. When used alone or in combination with tretinoin, the rates of complete remission have exceeded 85%, with high rates of molecular remission.

CONCLUSION

Arsenic trioxide, alone or in combination with tretinoin, as first-line therapy in newly diagnosed APL has resulted in high rates of complete remission and molecular remission. Arsenic trioxide combined with tretinoin has shortened the time to achieve complete remission and lengthened disease-free survival, findings that suggest the usefulness of the regimen as first-line treatment for APL.

摘要

目的

描述三氧化二砷作为治疗急性早幼粒细胞白血病(APL)一线药物的历史、临床药理学和毒性,以及其作用。

概述

APL 最常见的特征是 15 号和 17 号染色体之间的标志性相互易位,导致早幼粒细胞基因和维甲酸受体α融合。砷作为一种抗白血病药物的治疗效用最早在 18 世纪末被描述。三氧化二砷具有双重、剂量依赖性作用机制,既能诱导部分髓样分化,又能诱导凋亡。三氧化二砷通常耐受性良好,很少因可逆毒性而需要停止治疗。与三氧化二砷相关的毒性包括白细胞增多、Q-T 间期延长、APL 分化综合征和肝毒性。自 2000 年以来,三氧化二砷已被用作复发 APL 的标准治疗方法,单独使用时缓解率超过 80%。为了最大限度地提高 APL 患者的无病生存率并降低复发率,目前正在研究三氧化二砷作为 APL 治疗的一线治疗药物,多项研究显示出良好的结果。当单独使用或与维甲酸联合使用时,完全缓解率超过 85%,分子缓解率很高。

结论

三氧化二砷单独或与维甲酸联合作为新诊断 APL 的一线治疗药物,已导致完全缓解和分子缓解率很高。三氧化二砷与维甲酸联合使用可缩短达到完全缓解的时间并延长无病生存期,这表明该方案作为 APL 一线治疗的有用性。

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