形成原发性肿瘤异种移植物的能力可预测早期非小细胞肺癌疾病复发的风险增加。

The ability to form primary tumor xenografts is predictive of increased risk of disease recurrence in early-stage non-small cell lung cancer.

机构信息

Melbourne Centre for Clinical Sciences, Ludwig Institute for Cancer Research, Melbourne, Australia.

出版信息

Clin Cancer Res. 2011 Jan 1;17(1):134-41. doi: 10.1158/1078-0432.CCR-10-2224. Epub 2010 Nov 16.

DOI:10.1158/1078-0432.CCR-10-2224

PMID:21081655

Abstract

PURPOSE

Primary tumor xenografts (PTXG) established directly from patients' primary tumors in immunosuppressed animals might represent the spectrum of histologic complexity of lung cancers better than xenografts derived from established cell lines. These models are important in the study of aberrant biological pathways in cancers and as preclinical models for testing new therapeutic agents. However, not all primary tumors engraft when implanted into immunosuppressed mice. We have investigated factors that may influence the ability of primary non-small cell lung cancer (NSCLC) to form xenografts and their association with clinical outcome.

EXPERIMENTAL DESIGN

Tumor fragments from patients undergoing curative surgery were implanted into NOD-SCID (nonobese diabetic-severely combined immunodeficient) mice within 24 hours of surgery. Patient characteristics for tumors that engrafted (XG) and did not engraft (no-XG) were compared. Patient tumor DNA was profiled for the presence of 238 known mutations in 19 cancer-associated genes by using the MassARRAY platform.

RESULTS

Xenografts were established and passaged successfully from 63 of 157 (40%) implanted NSCLCs. Tumor factors associated with engraftment included squamous histology, poor differentiation, and larger tumor size. Significantly fewer EGFR (epidermal growth factor receptor)-mutated tumors engrafted (P = 0.03); conversely, more K-RAS-mutated tumors engrafted (P = 0.05). In multivariate analysis including age, sex, stage, and mutation, patients with XG tumors had significantly shorter disease-free survival compared with no-XG patients (hazard ratio: 7.0, 95% CI: 3.1-15.81; P < 0.000003).

CONCLUSION

PTXGs closely mirror the histology and molecular profiles of primary tumors and therefore may serve as important preclinical models. Tumors that engraft are biologically more aggressive and may be more representative of cancers with a higher propensity to relapse after surgery.

摘要

目的

直接从免疫抑制动物的患者原发肿瘤中建立的原发肿瘤异种移植物（PTXG）可能比从已建立的细胞系衍生的异种移植物更好地代表肺癌的组织学复杂性谱。这些模型在研究癌症中异常的生物学途径以及作为测试新治疗剂的临床前模型方面非常重要。然而，并非所有原发性肿瘤在植入免疫抑制小鼠时都会植入。我们已经研究了可能影响原发性非小细胞肺癌（NSCLC）形成异种移植物的能力的因素及其与临床结果的关联。

实验设计

在手术 24 小时内，将来自接受根治性手术的患者的肿瘤碎片植入 NOD-SCID（非肥胖型糖尿病-严重联合免疫缺陷）小鼠中。比较了植入（XG）和未植入（no-XG）的患者肿瘤特征。使用 MassARRAY 平台，对患者肿瘤 DNA 进行了 19 个癌症相关基因中 238 个已知突变的存在情况进行了分析。

结果

成功建立并传代了 157 个植入的 NSCLC 中的 63 个（40%）。与植入相关的肿瘤因素包括鳞状组织学、低分化和较大的肿瘤大小。表皮生长因子受体（EGFR）突变的肿瘤植入明显减少（P = 0.03）；相反，更多的 K-RAS 突变肿瘤植入（P = 0.05）。在包括年龄、性别、分期和突变在内的多变量分析中，XG 肿瘤患者的无病生存期明显短于 no-XG 患者（危险比：7.0，95%CI：3.1-15.81；P <0.000003）。