建立具有 EGFR、KRAS 和 FGFR1 遗传异常的患者来源的非小细胞肺癌异种移植模型:用于靶向治疗临床前研究的有用工具。
Establishment of patient-derived non-small cell lung cancer xenograft models with genetic aberrations within EGFR, KRAS and FGFR1: useful tools for preclinical studies of targeted therapies.
机构信息
Medical Research Center of Guangdong General Hospital & Guangdong Academy of Medical Sciences, Guangdong Lung Cancer Institute Guangzhou 510080, PR China.
出版信息
J Transl Med. 2013 Jul 10;11:168. doi: 10.1186/1479-5876-11-168.
BACKGROUND
Patient-derived tumor xenograft models have been established and increasingly used for preclinical studies of targeted therapies in recent years. However, patient-derived non-small cell lung cancer (NSCLC) xenograft mouse models are relatively few in number and are limited in their degree of genetic characterization and validation. In this study, we aimed to establish a variety of patient-derived NSCLC models and characterize these for common genetic aberrations to provide more informative models for preclinical drug efficacy testing.
METHODS
NSCLC tissues from thirty-one patients were collected and implanted into immunodeficient mice. Established xenograft models were characterized for common genetic aberrations, including detection of gene mutations within EGFR and KRAS, and genetic amplification of FGFR1 and cMET. Finally, gefitinib anti-tumor efficacy was tested in these patient-derived NSCLC xenograft models.
RESULTS
Ten passable patient-derived NSCLC xenograft models were established by implantation of NSCLC specimens of thirty-one patients into immunodeficient mice. Genetic aberrations were detected in six of the models, including one model with an EGFR activating mutation (Exon19 Del), one model with KRAS mutation, one model with both KRAS mutation and cMET gene amplification, and three models with FGFR1 amplification. Anti-tumor efficacy studies using gefitinib demonstrated that the EGFR activating mutation model had superior sensitivity and that the KRAS mutation models were resistant to gefitinib. The range of gefitinib responses in the patient-derived NSCLC xenograft models were consistent with the results reported from clinical trials. Furthermore, we observed that patient-derived NSCLC models with FGFR1 gene amplification were insensitive to gefitinib treatment.
CONCLUSIONS
Ten patient-derived NSCLC xenograft models were established containing a variety of genetic aberrations including EGFR activating mutation, KRAS mutation, and FGFR1 and cMET amplification. Gefitinib anti-tumor efficacy in these patient-derived NSCLC xenografts containing EGFR and KRAS mutation was consistent with the reported results from previous clinical trials. Thus, data from our panel of patient-derived NSCLC xenograft models confirms the utility of these models in furthering our understanding of this disease and aiding the development of personalized therapies for NSCLC patients.
背景
近年来,患者来源的肿瘤异种移植模型已被建立并越来越多地用于靶向治疗的临床前研究。然而,患者来源的非小细胞肺癌(NSCLC)异种移植小鼠模型数量相对较少,其遗传特征和验证程度有限。在这项研究中,我们旨在建立多种患者来源的 NSCLC 模型,并对这些模型进行常见遗传异常的特征分析,为临床前药物疗效测试提供更具信息性的模型。
方法
收集 31 名患者的 NSCLC 组织并植入免疫缺陷小鼠。对建立的异种移植模型进行常见遗传异常的特征分析,包括检测 EGFR 和 KRAS 内的基因突变,以及 FGFR1 和 cMET 的基因扩增。最后,在这些患者来源的 NSCLC 异种移植模型中测试吉非替尼的抗肿瘤疗效。
结果
通过将 31 名患者的 NSCLC 标本植入免疫缺陷小鼠,成功建立了 10 个可移植的患者来源的 NSCLC 异种移植模型。在 6 个模型中检测到遗传异常,包括一个具有 EGFR 激活突变(外显子 19 缺失)的模型、一个具有 KRAS 突变的模型、一个具有 KRAS 突变和 cMET 基因扩增的模型,以及三个具有 FGFR1 扩增的模型。使用吉非替尼进行的抗肿瘤疗效研究表明,具有 EGFR 激活突变的模型具有更高的敏感性,而具有 KRAS 突变的模型对吉非替尼耐药。患者来源的 NSCLC 异种移植模型中吉非替尼的反应范围与临床试验报告的结果一致。此外,我们观察到具有 FGFR1 基因扩增的患者来源的 NSCLC 模型对吉非替尼治疗不敏感。
结论
成功建立了 10 个包含多种遗传异常的患者来源的 NSCLC 异种移植模型,包括 EGFR 激活突变、KRAS 突变以及 FGFR1 和 cMET 扩增。这些患者来源的 NSCLC 异种移植模型中 EGFR 和 KRAS 突变的吉非替尼抗肿瘤疗效与之前临床试验报告的结果一致。因此,我们的患者来源的 NSCLC 异种移植模型的结果证实了这些模型在进一步了解该疾病和为 NSCLC 患者开发个性化治疗方面的实用性。
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