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RCC 的原位异种移植保留了患者肿瘤的组织学、免疫表型和遗传特征。

Orthotopic xenografts of RCC retain histological, immunophenotypic and genetic features of tumours in patients.

机构信息

Department of Pathology, Brigham and Women's Hospital, Harvard Medical School, Boston, MA, USA.

出版信息

J Pathol. 2011 Oct;225(2):212-21. doi: 10.1002/path.2929. Epub 2011 Jun 27.

Abstract

Renal cell carcinoma (RCC) is an aggressive malignancy with limited responsiveness to existing treatments. In vivo models of human cancer, including RCC, are critical for developing more effective therapies. Unfortunately, current RCC models do not accurately represent relevant properties of the human disease. The goal of this study was to develop clinically relevant animal models of RCC for preclinical investigations. We transplanted intact human tumour tissue fragments orthotopically in immunodeficient mice. The xenografts were validated by comparing the morphological, phenotypic and genetic characteristics of the kidney tumour tissues before and after implantation. Twenty kidney tumours were transplanted into mice. Successful tumour growth was detected in 19 cases (95%). The histopathological and immunophenotypic features of the xenografts and those of the original tumours largely overlapped in all cases. Evaluation of genetic alterations in a subset of 10 cases demonstrated that the grafts largely retained the genetic features of the pre-implantation RCC tissues. Indeed, primary tumours and corresponding grafts displayed identical VHL mutations. Moreover, an identical pattern of DNA copy amplification or loss was observed in 6/10 cases (60%). In summary, orthotopic engrafting of RCC tissue fragments can be successfully used to generate animal models that closely resemble RCC in patients. These models will be invaluable for in vivo preclinical drug testing and for deeper understanding of kidney carcinogenesis. The raw data of the SNP array analysis has been submitted to the GEO database (Accession No. GSE29062).

摘要

肾细胞癌(RCC)是一种侵袭性恶性肿瘤,对现有治疗方法的反应有限。包括 RCC 在内的人类癌症的体内模型对于开发更有效的治疗方法至关重要。不幸的是,目前的 RCC 模型不能准确地代表人类疾病的相关特性。本研究的目的是开发用于临床前研究的 RCC 临床相关动物模型。我们将完整的人肿瘤组织片段原位移植到免疫缺陷小鼠中。通过比较移植前后肾肿瘤组织的形态、表型和遗传特征来验证异种移植物。将 20 个肾肿瘤移植到小鼠中。在 19 例(95%)中成功检测到肿瘤生长。所有病例的异种移植物的组织病理学和免疫表型特征与原始肿瘤的特征大部分重叠。对 10 例亚组的遗传改变进行评估表明,移植物保留了移植前 RCC 组织的遗传特征。事实上,原发肿瘤和相应的移植物显示出相同的 VHL 突变。此外,在 6/10 例(60%)中观察到相同的 DNA 拷贝扩增或缺失模式。总之,RCC 组织片段的原位移植可成功用于生成与患者 RCC 非常相似的动物模型。这些模型将对体内临床前药物测试和深入了解肾癌发生具有重要价值。SNP 阵列分析的原始数据已提交给 GEO 数据库(注册号 GSE29062)。

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