[Current status and challenges of AML treatment with FLT3 inhibitors].

Yuichi Ishikawa
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Abstract

FLT3 mutation is one of the most frequent genetic mutations in AML, identified in approximately 30% of patients, and FLT3-ITD mutation is considered a poor prognostic factor. Based on these molecular and clinical backgrounds, FLT3 mutations are considered promising therapeutic targets in AML, and intensive development of targeted therapeutics has been ongoing for more than two decades. Recently, combination of FLT3 inhibitors with intensive chemotherapy for untreated AML patients with FLT3 mutations and FLT3 inhibitor monotherapy for relapsed/refractory patients have been approved. In Japan, the combination of quizartinib and intensive chemotherapy for untreated FLT3-ITD-positive AML was approved in 2023. Clinical use of FLT3 inhibitors shows strong promise for improving the clinical outcomes of these AML patients with an extremely poor prognosis. Meanwhile, various resistance mechanisms to FLT3 inhibitors have been identified, including the emergence of resistance-associated mutations, and attenuated inhibitory effects of FLT3 inhibitors involving the bone marrow microenvironment surrounding AML cells. Thus, future efforts should aim to optimize combination therapy based on the characteristics of each FLT3 inhibitor, develop biomarkers that could inform treatment selection, and to better understand these resistance mechanisms and develop methods for overcoming them.

[FLT3抑制剂治疗急性髓细胞白血病的现状与挑战]。
FLT3 突变是急性髓细胞性白血病最常见的基因突变之一,约有 30% 的患者发现了这种突变,而且 FLT3-ITD 突变被认为是一种不良预后因素。基于这些分子和临床背景,FLT3突变被认为是急性髓细胞性白血病有希望的治疗靶点,靶向治疗药物的深入开发已持续了二十多年。最近,FLT3 抑制剂联合强化化疗治疗未经治疗的 FLT3 突变急性髓细胞白血病患者,以及 FLT3 抑制剂单药治疗复发/难治性患者已获得批准。在日本,2023 年批准了奎沙替尼和强化化疗联合治疗未经治疗的 FLT3-ITD 阳性急性髓细胞白血病。FLT3抑制剂的临床应用为改善这些预后极差的急性髓细胞性白血病患者的临床预后带来了巨大希望。与此同时,FLT3 抑制剂的各种耐药机制也已被发现,包括耐药相关突变的出现,以及 AML 细胞周围骨髓微环境对 FLT3 抑制剂抑制作用的减弱。因此,未来的努力应着眼于根据每种FLT3抑制剂的特点优化联合疗法,开发可为治疗选择提供依据的生物标志物,以及更好地了解这些耐药机制并开发克服它们的方法。
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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