ASK12067(利莫替尼)通过抑制EGFR外显子20的插入发挥临床前抗肿瘤活性

Zhang Tao, Fang Feng, Lin-jiang Tong, Shingpan Chan, Yi Chen, Yan Li, Peiran Song, Yingqiang Liu, Gang Bai, Mengzhen Lai, Yi Ning, Yanan Wang, Yan-feng Fang, Zi-Xiang Pan, M. Geng, K. Ding, Jian Ding, Hua Xie
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摘要

表皮生长因子受体(EGFR)酪氨酸激酶抑制剂(TKIs)是癌症(NSCLC)患者个体化治疗的经典策略。然而,EGFR外显子20插入(EGFR 20ins)突变占NSCLC中所有EGFR突变病例的6%-12%,通常对可逆的EGFR TKI(如吉非替尼和埃罗替尼)具有耐药性,这使其成为癌症中具有挑战性的药物靶点。在我们之前的研究中,我们确定ASK12067(利默替尼)是一种新的第三代EGFR TKI,靶向EGFR T790M突变,具有良好的临床活性。在这里,我们获得了ASK12067对EGFR 20ins激活的效力,并评估了其对EGFR 20 ins驱动的肿瘤模型的体外和体内抗肿瘤活性。我们发现ASK12067对TKI抗性EGFR20ins激酶显示出强大的抑制活性。在TKI抗性EGFR 20ins依赖性BaF3细胞中,它剂量依赖性地抑制EGFR磷酸化,阻碍细胞增殖,并诱导细胞凋亡,其疗效远优于吉非替尼和埃洛替尼。此外,在EGFR 20in-BaF3异种移植物模型中,口服ASK120067降低了磷酸化EGFR 20ins的水平,并导致显著的肿瘤消退。这些结果显示了ASK12067在EGFR20ins模型中的临床前抗肿瘤疗效,并强调了ASK120067在治疗携带EGFR20ins突变的NSCLC患者方面的潜在价值。
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ASK120067 (limertinib) exerts pre-clinical anti-tumor activity by inhibiting EGFR exon20 insertion
Epidermal growth factor receptor (EGFR) tyrosine kinase inhibitors (TKIs) are classic strategies for the individualized treatment for patients with non-small cell lung cancer (NSCLC). However, EGFR exon20 insertion (EGFR 20ins) mutations, accounting for 6%–12% of all EGFR mutant cases in NSCLC, are generally resistant to the reversible EGFR TKIs (such as gefitinib and erlotinib), which makes them challenging drug-targets in lung cancer. In our previous study, we identified ASK120067 (limertinib) as a novel 3rd-generation EGFR TKI targeting EGFR T790M mutation with promising clinical activities. Here, we accessed the potency of ASK120067 on EGFR 20ins activation and evaluated its in vitro and in vivo anti-tumor activity against EGFR 20ins driven tumor models. We found that ASK120067 showed potent inhibitory activity on TKI-resistant EGFR 20ins kinase. In TKI-resistant EGFR 20ins-dependent BaF3 cells, it dose-dependently suppressed EGFR phosphorylation, impeded cell proliferation, and induced cell apoptosis with much superior efficacy to gefitinib and erlotinib. Moreover, oral administration of ASK120067 decreased the level of phospho-EGFR 20ins and caused significant tumor regression in EGFR 20ins BaF3 xenograft model. These results presented the pre-clinical anti-tumor efficacy of ASK120067 in EGFR 20ins models and highlighted the potential value of ASK120067 for the treatment of NSCLC patients harboring EGFR 20ins mutations.
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