新型FLT3抑制剂宁格替尼克服了急性髓性白血病的继发性耐药性。

IF 8.2 2区生物学 Q1 CELL BIOLOGY

Cell Communication and Signaling Pub Date : 2024-07-08 DOI:10.1186/s12964-024-01729-0

Chuhong Hu, Yvyin Zhang, Jie Yang, Yanli Xu, Tingfen Deng, Yumiao Li, Shilin Xu, Shunqing Wang, Peihong Wang

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引用次数: 0

摘要

背景：FMS样酪氨酸激酶3内部串联重复（FLT3-ITD）是急性髓性白血病（AML）中常见的突变类型，通常与患者预后不良有关。随着分子诊断技术的进步和酪氨酸激酶抑制剂（TKI）的开发，FLT3-ITD突变型AML患者的总生存期（OS）得到了一定程度的延长，但复发和耐药仍是巨大的挑战。宁格替尼是一种针对与肿瘤发病机制相关的多种激酶的新型TKI，目前正在进行肺癌的临床试验。本研究探讨了宁格替尼对FLT3突变的急性髓细胞白血病的体内和体外抗肿瘤活性：方法：在表达各种 FLT3 突变的 AML 细胞系和 Ba/F3 细胞中进行细胞增殖试验，以验证宁格替尼在体外的抗白血病活性。免疫印迹试验用于验证宁格替尼对 FLT3 蛋白和下游通路的影响。分子对接和CETSA用于验证宁格替尼与靶蛋白的相互作用。在Ba/F3-FLT3-ITD-、MOLM13、Ba/F3-FLT3-ITD-F691L-、MOLM13-FLT3-ITD-F691L诱导的白血病小鼠模型中评估了宁格替尼的体内生存益处。我们还使用了源自患者的原代细胞来确定宁格替尼的疗效：结果：在FLT3-ITD AML细胞系中，宁格替尼抑制细胞增殖、阻滞细胞周期、诱导细胞凋亡，并结合FLT3抑制其下游信号通路，包括STAT5、AKT和ERK通路。在FLT3-ITD和FLT3-ITD-F691L突变的小鼠模型中，宁格替尼显示出优于现有临床药物吉特替尼和奎扎替尼的抗白血病活性，显著延长了小鼠的生存期。此外，宁格替尼对携带FLT3-ITD突变的患者原代细胞也有活性：总之，我们的研究证实了宁格替尼在FLT3-ITD突变的急性髓细胞性白血病中的治疗作用，为临床耐药患者提供了一种潜在的新选择。

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Ningetinib, a novel FLT3 inhibitor, overcomes secondary drug resistance in acute myeloid leukemia.

Background: FMS-like tyrosine kinase 3 internal tandem duplication (FLT3-ITD) is a common mutation type in acute myeloid leukemia (AML) and is usually associated with poor patient prognosis. With advancements in molecular diagnostics and the development of tyrosine kinase inhibitors (TKI), the overall survival (OS) of AML patients with FLT3-ITD mutations has been prolonged to some extent, but relapse and drug resistance are still substantial challenges. Ningetinib is a novel TKI against various kinases in relation to tumour pathogenesis and is undergoing clinical trials of lung cancer. In this study, we explored the antitumor activity of ningetinib against AML with FLT3 mutations both in vivo and in vitro.

Methods: Cell proliferation assays were performed in AML cell lines and Ba/F3 cells expressing various FLT3 mutations to validate the antileukemic activity of ningetinib in vitro. Immunoblot assays were used to verify the effect of ningetinib on the FLT3 protein and downstream pathways. Molecular docking and CETSA were used to validate the interaction of ningetinib with target proteins. The survival benefit of ningetinib in vivo was assessed in Ba/F3-FLT3-ITD-, MOLM13, Ba/F3-FLT3-ITD-F691L-, MOLM13-FLT3-ITD-F691L-induced leukemia mouse models. We also used patient-derived primary cells to determine the efficacy of ningetinib.

Results: Ningetinib inhibited cell proliferation, blocked the cell cycle, induced apoptosis and bound FLT3 to inhibit its downstream signaling pathways, including the STAT5, AKT and ERK pathways, in FLT3-ITD AML cell lines. In the mouse models with FLT3-ITD and FLT3-ITD-F691L mutation, ningetinib showed superior anti-leukemia activity to existing clinical drugs gilteritinib and quizartinib, significantly prolongating the survival of mice. In addition, ningetinib exhibited activity against patient-derived primary cells harboring FLT3-ITD mutations.

Conclusion: Overall, our study confirmed the therapeutic role of ningetinib in AML with FLT3-ITD mutations, providing a potential new option for clinically resistant patients.

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来源期刊

Cell Communication and Signaling CELL BIOLOGY-

CiteScore

11.00

自引率

0.00%

发文量

180

期刊介绍： Cell Communication and Signaling (CCS) is a peer-reviewed, open-access scientific journal that focuses on cellular signaling pathways in both normal and pathological conditions. It publishes original research, reviews, and commentaries, welcoming studies that utilize molecular, morphological, biochemical, structural, and cell biology approaches. CCS also encourages interdisciplinary work and innovative models, including in silico, in vitro, and in vivo approaches, to facilitate investigations of cell signaling pathways, networks, and behavior. Starting from January 2019, CCS is proud to announce its affiliation with the International Cell Death Society. The journal now encourages submissions covering all aspects of cell death, including apoptotic and non-apoptotic mechanisms, cell death in model systems, autophagy, clearance of dying cells, and the immunological and pathological consequences of dying cells in the tissue microenvironment.