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A Versatile Orthotopic Nude Mouse Model for Study of Esophageal Squamous Cell Carcinoma

机译:一种用于研究食管鳞状细胞癌的多功能原位裸小鼠模型

摘要

Increasing evidence indicates tumor-stromal interactions play a crucial role in cancer. An in vivo esophageal squamous cell carcinoma (ESCC) orthotopic animal model was developed with bioluminescence imaging established with a real-time monitoring platform for functional and signaling investigation of tumor-stromal interactions. The model was produced by injection of luciferase-labelled ESCC cells into the intraesophageal wall of nude mice. Histological examination indicates this orthotopic model is highly reproducible with 100% tumorigenesis among the four ESCC cell lines tested. This new model recapitulates many clinical and pathological properties of human ESCC, including esophageal luminal stricture by squamous cell carcinoma with nodular tumor growth, adventitia invasion, lymphovascular invasion, and perineural infiltration. It was tested using an AKT shRNA knockdown of ESCC cell lines and the in vivo tumor suppressive effects of AKT knockdown were observed. In conclusion, this ESCC orthotopic mouse model allows investigation of gene functions of cancer cells in a more natural tumor microenvironment and has advantages over previous established models. It provides a versatile platform with potential application for metastasis and therapeutic regimen testing.
机译:越来越多的证据表明,肿瘤与基质之间的相互作用在癌症中起着至关重要的作用。利用生物发光成像技术开发了体内食管鳞状细胞癌(ESCC)原位动物模型,并建立了实时监测平台,用于功能和信号传导研究肿瘤间质相互作用。该模型是通过将荧光素酶标记的ESCC细胞注射到裸鼠的食管内壁而产生的。组织学检查表明,该原位模型可高度重现,在所测试的四种ESCC细胞系中具有100%的致瘤性。这种新模型概括了人类ESCC的许多临床和病理学特征,包括鳞状细胞癌伴结节性肿瘤生长,外膜浸润,淋巴血管浸润和神经周浸润引起的食管腔狭窄。使用ESCC细胞系的AKT shRNA敲除测试了它,并且观察到AKT敲除的体内肿瘤抑制作用。总之,此ESCC原位小鼠模型允许在更自然的肿瘤微环境中研究癌细胞的基因功能,并且比以前建立的模型具有优势。它为转移和治疗方案测试提供了潜在的多功能平台。

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