Discovery and Preclinical Research Division, Taiho Pharmaceutical Co., Ltd., Tsukuba, Ibaraki, Japan.
Department of Surgical Oncology Molecular Oncology and Therapeutics, Osaka City University Graduate School of Medicine, Osaka, Japan.
Cancer Res. 2020 Nov 15;80(22):4986-4997. doi: 10.1158/0008-5472.CAN-19-2568. Epub 2020 Sep 24.
FGFR signaling is deregulated in many human cancers, and FGFR is considered a valid target in FGFR-deregulated tumors. Here, we examine the preclinical profile of futibatinib (TAS-120; 1-[(3S)-[4-amino-3-[(3,5-dimethoxyphenyl)ethynyl]-1H-pyrazolo[3, 4-d] pyrimidin-1-yl]-1-pyrrolidinyl]-2-propen-1-one), a structurally novel, irreversible FGFR1-4 inhibitor. Among a panel of 296 human kinases, futibatinib selectively inhibited FGFR1-4 with IC values of 1.4 to 3.7 nmol/L. Futibatinib covalently bound the FGFR kinase domain, inhibiting FGFR phosphorylation and, in turn, downstream signaling in FGFR-deregulated tumor cell lines. Futibatinib exhibited potent, selective growth inhibition of several tumor cell lines (gastric, lung, multiple myeloma, bladder, endometrial, and breast) harboring various genomic aberrations. Oral administration of futibatinib led to significant dose-dependent tumor reduction in various FGFR-driven human tumor xenograft models, and tumor reduction was associated with sustained FGFR inhibition, which was proportional to the administered dose. The frequency of appearance of drug-resistant clones was lower with futibatinib than a reversible ATP-competitive FGFR inhibitor, and futibatinib inhibited several drug-resistant FGFR2 mutants, including the FGFR2 V565I/L gatekeeper mutants, with greater potency than any reversible FGFR inhibitors tested (IC, 1.3-50.6 nmol/L). These results indicate that futibatinib is a novel orally available, potent, selective, and irreversible inhibitor of FGFR1-4 with a broad spectrum of antitumor activity in cell lines and xenograft models. These findings provide a strong rationale for testing futibatinib in patients with tumors oncogenically driven by FGFR genomic aberrations, with phase I to III trials ongoing. SIGNIFICANCE: Preclinical characterization of futibatinib, an irreversible FGFR1-4 inhibitor, demonstrates selective and potent antitumor activity against FGFR-deregulated cancer cell lines and xenograft models, supporting clinical evaluation in patients with FGFR-driven tumors. GRAPHICAL ABSTRACT: http://cancerres.aacrjournals.org/content/canres/80/22/4986/F1.large.jpg.
FGFR 信号在许多人类癌症中失调,FGFR 被认为是 FGFR 失调肿瘤的有效靶点。在这里,我们研究了 futibatinib(TAS-120;1-[(3S)-[4-氨基-3-[(3,5-二甲氧基苯基)乙炔基]-1H-吡唑并[3,4-d]嘧啶-1-基]-1-吡咯烷基]-2-丙烯-1-酮)的临床前特征,这是一种结构新颖的不可逆 FGFR1-4 抑制剂。在 296 个人类激酶的面板中,futibatinib 选择性地抑制 FGFR1-4,IC 值为 1.4 至 3.7 nmol/L。Futibatinib 与 FGFR 激酶结构域共价结合,抑制 FGFR 磷酸化,进而抑制 FGFR 失调肿瘤细胞系的下游信号转导。Futibatinib 对多种肿瘤细胞系(胃、肺、多发性骨髓瘤、膀胱、子宫内膜和乳腺)具有选择性的生长抑制作用,这些细胞系存在各种基因组异常。口服 futibatinib 可导致各种 FGFR 驱动的人肿瘤异种移植模型中的肿瘤显著剂量依赖性减少,并且肿瘤减少与持续的 FGFR 抑制相关,这与给予的剂量成正比。与可逆的 ATP 竞争性 FGFR 抑制剂相比,futibatinib 出现耐药克隆的频率较低,并且 futibatinib 抑制了几种耐药性 FGFR2 突变体,包括 FGFR2 V565I/L 门控突变体,其效力高于任何测试过的可逆 FGFR 抑制剂(IC,1.3-50.6 nmol/L)。这些结果表明,futibatinib 是一种新型的口服有效、强效、选择性和不可逆的 FGFR1-4 抑制剂,在细胞系和异种移植模型中具有广谱的抗肿瘤活性。这些发现为在 FGFR 基因组异常驱动的肿瘤患者中测试 futibatinib 提供了强有力的理由,目前正在进行 I 期至 III 期试验。意义:不可逆 FGFR1-4 抑制剂 futibatinib 的临床前特征表明,对 FGFR 失调的癌细胞系和异种移植模型具有选择性和强大的抗肿瘤活性,支持在 FGFR 驱动的肿瘤患者中进行临床评估。
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