高三尖杉酯碱通过合成致死效应与FLT3-ITD急性髓系白血病选择性靶向的合理组合。
Rational combination of homoharringtonine to selectively target FLT3-ITD acute myeloid leukemia through synthetic lethality.
作者信息
Li Ying, Gao Xiaoxiao, Zhang Huimin, Qiu Yang, Chai Meng, Liu Jinghua, Yan Xiaojing, Waxman Samuel, Zhang Jingyi, Jing Yongkui
机构信息
Liaoning Key Lab of Targeting Drugs for Hematological Malignancies, Department of Pharmacology, Shenyang Pharmaceutical University, Shenyang 110016, PR China.
Department of Hematology, Northern Theater General Hospital, Shenyang 110016, PR China.
出版信息
Phytomedicine. 2025 Oct;146:157124. doi: 10.1016/j.phymed.2025.157124. Epub 2025 Jul 29.
BACKGROUND
Homoharringtonine (HHT), a natural product used clinically to treat acute myeloid leukemia (AML) in combination with chemotherapy, induced transient remission in 25 % of unclassified AML patients when administered alone. Recent studies showed that HHT could be combined with targeting agents for AML treatment. However, the rationales of these combinations require further exploration to optimize therapeutic efficacy.
PURPOSE
To explore the sensitive subgroup of AML cells to HHT and to evaluate its optimal combinations with FLT3-ITD or Bcl-2 inhibitors based on apoptosis induction.
METHODS
AML cell lines harboring FLT3-ITD mutation and wild-type FLT3 were used to compare the apoptosis induction of HHT alone and in combination with venetoclax or FLT3-ITD inhibitor. siRNA and Western blotting were used to identify the key factors in the apoptosis induction. Xenograft models were used to test the in vivo antileukemia efficacy and toxicity.
RESULTS
FLT3-ITD AML cell lines and primary AML cells exhibited greater sensitivity to HHT-induced apoptosis and in vivo antileukemia effects than FLT3 wild-type cells. HHT induces apoptosis through repressing the antiapoptotic protein Mcl-1 and activating the proapoptotic protein Bax, which is attenuated by Mcl-1 overexpression and Bax knockdown. HHT in combination with Bcl-2 inhibitor venetoclax induce synergistic apoptosis across all cell lines with enhanced toxicity observed in vivo. HHT plus FLT3 inhibitors, including midostaurin, quizartinib, gilteritinib and sorafenib, induce selective synergistic apoptosis in FLT3-ITD AML cells, with the most potent effect observed in the combination of HHT and quizartinib. HHT plus quizartinib significantly prolonged FLT3-ITD AML xenograft survival without causing toxicity.
CONCLUSIONS
FLT3-ITD AML cells represent a responsive subgroup to HHT treatment in vitro and in vivo. The combination of HHT and quizartinib demonstrates optimal efficacy and selectivity against FLT3-ITD AML cells in xenografts, with no observed toxicity.
背景
高三尖杉酯碱(HHT)是一种临床上与化疗联合用于治疗急性髓系白血病(AML)的天然产物,单独使用时可使25%的未分类AML患者获得短暂缓解。最近的研究表明,HHT可与靶向药物联合用于AML治疗。然而,这些联合用药的原理需要进一步探索以优化治疗效果。
目的
探索AML细胞对HHT敏感的亚组,并基于诱导凋亡评估其与FLT3-ITD或Bcl-2抑制剂的最佳联合用药方案。
方法
使用携带FLT3-ITD突变的AML细胞系和野生型FLT3的AML细胞系,比较HHT单独使用以及与维奈克拉或FLT3-ITD抑制剂联合使用时诱导凋亡的情况。使用小干扰RNA(siRNA)和蛋白质免疫印迹法来鉴定诱导凋亡的关键因子。使用异种移植模型来测试体内抗白血病疗效和毒性。
结果
与FLT3野生型细胞相比,FLT3-ITD AML细胞系和原发性AML细胞对HHT诱导的凋亡和体内抗白血病作用表现出更高的敏感性。HHT通过抑制抗凋亡蛋白Mcl-1和激活促凋亡蛋白Bax来诱导凋亡,而Mcl-1过表达和Bax基因敲低可减弱这种作用。HHT与Bcl-2抑制剂维奈克拉联合使用可在所有细胞系中诱导协同凋亡,且在体内观察到毒性增强。HHT加FLT3抑制剂,包括米哚妥林、奎扎替尼、吉瑞替尼和索拉非尼,可在FLT3-ITD AML细胞中诱导选择性协同凋亡,其中HHT与奎扎替尼联合使用时效果最为显著。HHT加奎扎替尼可显著延长FLT3-ITD AML异种移植瘤的生存期且不产生毒性。
结论
FLT3-ITD AML细胞在体外和体内均是对HHT治疗有反应的亚组。HHT与奎扎替尼联合使用在异种移植瘤中对FLT3-ITD AML细胞显示出最佳疗效和选择性,且未观察到毒性。
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