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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >A cellular model reflecting the phenotypic heterogeneity of mutant HRAS driven squamous cell carcinoma
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A cellular model reflecting the phenotypic heterogeneity of mutant HRAS driven squamous cell carcinoma

机译:反映突变HRAS驱动的鳞状细胞癌表型异质性的细胞模型

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Squamous cell carcinomas have a range of histopathological manifestations. The parameters that determine this clinically observed heterogeneity are not fully understood. Here, we report the generation of a cell culture model that reflects part of this heterogeneity. We have used the catalytic subunit of human telomerase hTERT and large T to immortalize primary UV-unexposed keratinocytes. Then, mutant HRAS G12V has been introduced to transform these immortal keratinocytes. When injected into immunosuppressed mice, transformed cells grew as xenografts with distinct histopathological characteristics. We observed three major tissue architectures: solid, sarcomatoid and cystic growth types, which were primarily composed of pleomorphic and basaloid cells but in some cases displayed focal apocrine differentiation. We demonstrate that the cells generated represent different stages of skin cancerogenesis and as such can be used to identify novel tumor-promoting alterations such as the overexpression of the PADI2 oncogene in solid-type SCC. Importantly, the cultured cells maintain the characteristics from the xenograft they were derived from while being amenable to manipulation and analysis. The availability of cell lines representing different clinical manifestations opens a new tool to study the stochastic and deterministic factors that cause case-to-case heterogeneity despite departing from the same set of oncogenes and the same genetic background.
机译:鳞状细胞癌具有多种组织病理学表现。尚未完全了解确定此临床观察到的异质性的参数。在这里,我们报告了反映部分这种异质性的细胞培养模型的生成。我们已使用人类端粒酶hTERT和大T的催化亚基来永生未暴露于紫外线的角质形成细胞。然后,已引入突变体HRAS G12V来转化这些永生的角质形成细胞。当注射到免疫抑制的小鼠中时,转化的细胞以异种移植物的形式生长,具有独特的组织病理学特征。我们观察到了三种主要的组织结构:实体,肉瘤样和囊性生长类型,它们主要由多形和基底细胞组成,但在某些情况下表现出局灶性主分泌分化。我们证明生成的细胞代表皮肤癌发生的不同阶段,因此可用于鉴定新型肿瘤促进性改变,例如在固态SCC中过表达PADI2癌基因。重要的是,培养的细胞保持了来自它们的异种移植物的特性,同时可以进行操纵和分析。代表不同临床表现的细胞系的可用性为研究导致病例间异质性的随机和确定性因素打开了一个新工具,尽管这些因素来自相同的致癌基因组和相同的遗传背景。

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