FDA-approved disulfiram as a novel treatment for aggressive leukemia.

IF 4.8 3区医学 Q1 GENETICS & HEREDITY

Journal of Molecular Medicine-Jmm Pub Date : 2024-04-01 Epub Date: 2024-02-13 DOI:10.1007/s00109-023-02414-4

Mawar Karsa, Lin Xiao, Emma Ronca, Angelika Bongers, Dayna Spurling, Ayu Karsa, Sandra Cantilena, Anna Mariana, Tim W Failes, Greg M Arndt, Laurence C Cheung, Rishi S Kotecha, Rosemary Sutton, Richard B Lock, Owen Williams, Jasper de Boer, Michelle Haber, Murray D Norris, Michelle J Henderson, Klaartje Somers

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引用次数: 0

Abstract

Acute leukemia continues to be a major cause of death from disease worldwide and current chemotherapeutic agents are associated with significant morbidity in survivors. While better and safer treatments for acute leukemia are urgently needed, standard drug development pipelines are lengthy and drug repurposing therefore provides a promising approach. Our previous evaluation of FDA-approved drugs for their antileukemic activity identified disulfiram, used for the treatment of alcoholism, as a candidate hit compound. This study assessed the biological effects of disulfiram on leukemia cells and evaluated its potential as a treatment strategy. We found that disulfiram inhibits the viability of a diverse panel of acute lymphoblastic and myeloid leukemia cell lines (n = 16) and patient-derived xenograft cells from patients with poor outcome and treatment-resistant disease (n = 15). The drug induced oxidative stress and apoptosis in leukemia cells within hours of treatment and was able to potentiate the effects of daunorubicin, etoposide, topotecan, cytarabine, and mitoxantrone chemotherapy. Upon combining disulfiram with auranofin, a drug approved for the treatment of rheumatoid arthritis that was previously shown to exert antileukemic effects, strong and consistent synergy was observed across a diverse panel of acute leukemia cell lines, the mechanism of which was based on enhanced ROS induction. Acute leukemia cells were more sensitive to the cytotoxic activity of disulfiram than solid cancer cell lines and non-malignant cells. While disulfiram is currently under investigation in clinical trials for solid cancers, this study provides evidence for the potential of disulfiram for acute leukemia treatment. KEY MESSAGES: Disulfiram induces rapid apoptosis in leukemia cells by boosting oxidative stress. Disulfiram inhibits leukemia cell growth more potently than solid cancer cell growth. Disulfiram can enhance the antileukemic efficacy of chemotherapies. Disulfiram strongly synergises with auranofin in killing acute leukemia cells by ROS induction. We propose testing of disulfiram in clinical trial for patients with acute leukemia.

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美国食品和药物管理局批准将双硫仑作为治疗侵袭性白血病的新型疗法。

急性白血病仍然是全球疾病致死的主要原因，而目前的化疗药物与幸存者的严重发病率有关。虽然急性白血病急需更好、更安全的治疗方法，但标准药物开发流程漫长，因此药物再利用提供了一种很有前景的方法。我们之前对美国食品及药物管理局批准的药物进行了抗白血病活性评估，发现用于治疗酒精中毒的双硫仑是一种候选热门化合物。本研究评估了双硫仑对白血病细胞的生物效应，并评估了其作为治疗策略的潜力。我们发现，双硫仑能抑制多种急性淋巴细胞白血病和骨髓性白血病细胞系（n = 16）以及来自疗效不佳和耐药患者的异种移植细胞（n = 15）的活力。这种药物能在治疗后数小时内诱导白血病细胞产生氧化应激和凋亡，并能增强达乌比星、依托泊苷、拓扑替康、阿糖胞苷和米托蒽醌化疗的效果。在将双硫仑与欧拉诺芬（一种已被批准用于治疗类风湿性关节炎的药物，以前曾被证明具有抗白血病作用）结合使用时，在不同的急性白血病细胞系中观察到了强烈而一致的协同作用，其机制是基于增强的 ROS 诱导。与实体癌细胞系和非恶性细胞相比，急性白血病细胞对双硫仑的细胞毒性活性更为敏感。尽管目前正在对双硫仑治疗实体癌的临床试验进行调查，但这项研究为双硫仑治疗急性白血病的潜力提供了证据。关键信息：双硫仑通过增强氧化应激诱导白血病细胞快速凋亡。双硫仑抑制白血病细胞生长的作用比抑制实体癌细胞生长的作用更强。双硫仑能增强化疗药物的抗白血病疗效。在通过诱导 ROS 杀死急性白血病细胞方面，二硫仑与呋喃妥因具有很强的协同作用。我们建议在急性白血病患者的临床试验中试用双硫仑。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Molecular Medicine-Jmm 医学-医学：研究与实验

CiteScore

9.30

自引率

0.00%

发文量

100

审稿时长

1.3 months

期刊介绍： The Journal of Molecular Medicine publishes original research articles and review articles that range from basic findings in mechanisms of disease pathogenesis to therapy. The focus includes all human diseases, including but not limited to: Aging, angiogenesis, autoimmune diseases as well as other inflammatory diseases, cancer, cardiovascular diseases, development and differentiation, endocrinology, gastrointestinal diseases and hepatology, genetics and epigenetics, hematology, hypoxia research, immunology, infectious diseases, metabolic disorders, neuroscience of diseases, -omics based disease research, regenerative medicine, and stem cell research. Studies solely based on cell lines will not be considered. Studies that are based on model organisms will be considered as long as they are directly relevant to human disease.