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由EGFR-T790M或EGFR-C797S介导的靶向耐药对EGFR外显子20插入突变活性酪氨酸激酶抑制剂的影响。

The Impact of On-Target Resistance Mediated by EGFR-T790M or EGFR-C797S on EGFR Exon 20 Insertion Mutation Active Tyrosine Kinase Inhibitors.

作者信息

Kobayashi Ikei S, Shaffer William, Viray Hollis, Rangachari Deepa, VanderLaan Paul A, Kobayashi Susumu S, Costa Daniel B

机构信息

Division of Medical Oncology, Department of Medicine, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, Massachusetts.

Department of Pathology, Beth Israel Deaconess Medical Center, Boston, Massachusetts.

出版信息

JTO Clin Res Rep. 2023 Nov 27;5(1):100614. doi: 10.1016/j.jtocrr.2023.100614. eCollection 2024 Jan.

DOI:10.1016/j.jtocrr.2023.100614
PMID:38229766
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10788275/
Abstract

INTRODUCTION

Mechanisms of resistance to EGFR exon 20 insertion mutation active inhibitors have not been extensively studied in either robust preclinical models or patient-derived rebiopsy specimens. We sought to characterize on-target resistance mutations identified in exon 20 insertion-mutated lung cancers treated with mobocertinib or poziotinib and evaluate whether these mutations would or would not have cross-resistance to next-generation inhibitors zipalertinib, furmonertinib, and sunvozertinib.

METHODS

We identified mechanisms of resistance to EGFR exon 20 insertion mutation active inhibitors and then used preclinical models of EGFR exon 20 insertion mutations (A767_V769dupASV, D770_N771insSVD, V773_C774insH) plus common EGFR mutants to probe inhibitors in the absence/presence of EGFR-T790M or EGFR-C797S.

RESULTS

Mobocertinib had a favorable therapeutic window in relation to EGFR wild type for EGFR exon 20 insertion mutants, but the addition of EGFR-T790M or EGFR-C797S negated the observed window. Zipalertinib had a favorable therapeutic window for cells driven by EGFR-A767_V769dupASV or EGFR-D770_N771insSVD in the presence or absence of EGFR-T790M. Furmonertinib and sunvozertinib had the most favorable therapeutic windows in the presence or absence of EGFR-T790M in all cells tested. -C797S in to all mutations evaluated generated dependent cells that were resistant to the covalent EGFR tyrosine kinase inhibitors mobocertinib, zipalertinib, furmonertinib, sunvozertinib, poziotinib, and osimertinib.

CONCLUSIONS

This report highlights that poziotinib and mobocertinib are susceptible to on-target resistance mediated by -T790M or -C797S in the background of the most prevalent EGFR exon 20 insertion mutations. Furmonertinib, sunvozertinib, and to a less extent zipalertinib can overcome EGFR-T790M compound mutants, whereas EGFR-C797S leads to covalent inhibitor cross-resistance-robust data that support the limitations of mobocertinib and should further spawn the development of next-generation covalent and reversible EGFR exon 20 insertion mutation active inhibitors with favorable therapeutic windows that are less vulnerable to on-target resistance.

摘要

引言

在强大的临床前模型或患者来源的再活检标本中,对表皮生长因子受体(EGFR)外显子20插入突变活性抑制剂的耐药机制尚未得到广泛研究。我们试图对在用莫博替尼或波齐替尼治疗的外显子20插入突变型肺癌中鉴定出的靶向耐药突变进行特征分析,并评估这些突变对下一代抑制剂齐帕替尼、伏美替尼和舒沃替尼是否具有交叉耐药性。

方法

我们确定了对EGFR外显子20插入突变活性抑制剂的耐药机制,然后使用EGFR外显子20插入突变(A767_V769dupASV、D770_N771insSVD、V773_C774insH)加常见EGFR突变体的临床前模型,在不存在/存在EGFR-T790M或EGFR-C-797S的情况下检测抑制剂。

结果

对于EGFR外显子20插入突变体,莫博替尼相对于EGFR野生型具有良好的治疗窗口,但添加EGFR-T790M或EGFR-C797S会消除观察到的窗口。在存在或不存在EGFR-T790M的情况下,齐帕替尼对由EGFR-A767_V769dupASV或EGFR-D770_N771insSVD驱动的细胞具有良好的治疗窗口。在所有测试细胞中,无论是否存在EGFR-T790M,伏美替尼和舒沃替尼都具有最良好的治疗窗口。在评估的所有突变中,EGFR-C797S产生了对共价EGFR酪氨酸激酶抑制剂莫博替尼、齐帕替尼伏美替尼、舒沃替尼、波齐替尼和奥希替尼耐药的依赖性细胞。

结论

本报告强调,在最常见的EGFR外显子20插入突变背景下,波齐替尼和莫博替尼易受EGFR-T790M或EGFR-C797S介导的靶向耐药影响。伏美替尼、舒沃替尼,以及程度较轻的齐帕替尼可以克服EGFR-T790M复合突变体,而EGFR-C797S导致共价抑制剂交叉耐药——这些有力的数据支持了莫博替尼的局限性,并应进一步推动开发具有良好治疗窗口、不易受到靶向耐药影响的下一代共价和可逆EGFR外显子20插入突变活性抑制剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fa2c/10788275/badc7f6695e1/gr1.jpg

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