MUC1-C Is a Common Driver of Acquired Osimertinib Resistance in NSCLC

IF 21 1区 医学 Q1 ONCOLOGY Journal of Thoracic Oncology Pub Date : 2024-03-01 DOI:10.1016/j.jtho.2023.10.017
Naoki Haratake MD, PhD , Hiroki Ozawa MD, PhD , Yoshihiro Morimoto MD, PhD , Nami Yamashita MD, PhD , Tatsuaki Daimon MD, PhD , Atrayee Bhattacharya PhD , Keyi Wang MD , Ayako Nakashoji MD, PhD , Hideko Isozaki PhD , Mototsugu Shimokawa PhD , Chie Kikutake PhD , Mikita Suyama PhD , Asato Hashinokuchi MD , Kazuki Takada MD, PhD , Tomoyoshi Takenaka MD, PhD , Tomoharu Yoshizumi MD, PhD , Tetsuya Mitsudomi MD, PhD , Aaron N. Hata MD, PhD , Donald Kufe MD
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Abstract

Introduction

Osimertinib is an irreversible EGFR tyrosine kinase inhibitor approved for the first-line treatment of patients with metastatic NSCLC harboring EGFR exon 19 deletions or L858R mutations. Patients treated with osimertinib invariably develop acquired resistance by mechanisms involving additional EGFR mutations, MET amplification, and other pathways. There is no known involvement of the oncogenic MUC1-C protein in acquired osimertinib resistance.

Methods

H1975/EGFR (L858R/T790M) and patient-derived NSCLC cells with acquired osimertinib resistance were investigated for MUC1-C dependence in studies of EGFR pathway activation, clonogenicity, and self-renewal capacity.

Results

We reveal that MUC1-C is up-regulated in H1975 osimertinib drug-tolerant persister cells and is necessary for activation of the EGFR pathway. H1975 cells selected for stable osimertinib resistance (H1975-OR) and MGH700-2D cells isolated from a patient with acquired osimertinib resistance are found to be dependent on MUC1-C for induction of (1) phospho (p)-EGFR, p-ERK, and p-AKT, (2) EMT, and (3) the resistant phenotype. We report that MUC1-C is also required for p-EGFR, p-ERK, and p-AKT activation and self-renewal capacity in acquired osimertinib-resistant (1) MET-amplified MGH170-1D #2 cells and (2) MGH121 Res#2/EGFR (T790M/C797S) cells. Importantly, targeting MUC1-C in these diverse models reverses osimertinib resistance. In support of these results, high MUC1 mRNA and MUC1-C protein expression is associated with a poor prognosis for patients with EGFR-mutant NSCLCs.

Conclusions

Our findings reveal that MUC1-C is a common effector of osimertinib resistance and is a potential target for the treatment of osimertinib-resistant NSCLCs.

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MUC1-C是非小细胞肺癌获得性奥西替尼耐药性的常见驱动因素。
背景:Osimertinib是一种不可逆的EGFR酪氨酸激酶抑制剂,被批准用于一线治疗携带EGFR外显子19缺失或L858R突变的转移性NSCLC患者。奥西替尼治疗的患者总是通过涉及额外EGFR突变、MET扩增和其他途径的机制产生获得性耐药性。目前还没有已知致癌MUC1-C蛋白参与获得性奥西替尼耐药性。方法:对H1975/EGFR(L858R/T790M)和具有获得性奥西替尼耐药性的患者来源的NSCLC细胞的MUC1-C依赖性进行研究,以研究EGFR通路的激活、克隆发生性和自我更新能力。结果:我们证明MUC1-C在H1975奥西替尼药物耐受性persister(DTP)细胞中上调,并且是激活EGFR途径所必需的。从具有获得性奥西替尼抗性的患者中分离的用于稳定奥西替尼抗性的H1975细胞(H1975-OR)和MGH700-2D细胞显示依赖于MUC1-C来诱导(i)p-EGFR、p-ERK和p-AKT,(ii)EMT,和(iii)抗性表型。我们报道,在获得性奥西替尼抗性(i)MET扩增的MGH170-1D#2细胞和(ii)MGH121-Res#2/EGFR(T790M/C797S)细胞中,MUC1-C也是p-EGFR、p-ERK和p-AKT激活和自我更新能力所必需的。重要的是,在这些不同的模型中靶向MUC1-C可以逆转奥西替尼的耐药性。为了支持这些结果,高MUC1mRNA和MUC1-C蛋白表达与EGFR突变NSCLC患者的不良预后相关。结论:我们的研究结果表明,MUC1-C是奥西替尼耐药性的常见效应物,是治疗奥西替尼非小细胞肺癌的潜在靶点。
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来源期刊
Journal of Thoracic Oncology
Journal of Thoracic Oncology 医学-呼吸系统
CiteScore
36.00
自引率
3.90%
发文量
1406
审稿时长
13 days
期刊介绍: Journal of Thoracic Oncology (JTO), the official journal of the International Association for the Study of Lung Cancer,is the primary educational and informational publication for topics relevant to the prevention, detection, diagnosis, and treatment of all thoracic malignancies.The readship includes epidemiologists, medical oncologists, radiation oncologists, thoracic surgeons, pulmonologists, radiologists, pathologists, nuclear medicine physicians, and research scientists with a special interest in thoracic oncology.
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