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小鼠肿瘤模型ER 15-P中形态学异质性和表型不稳定性与转移稳定性的对比

Morphological heterogeneity and phenotypical instability versus metastatic stability in the murine tumor model ER 15-P.

作者信息

Edel G, Roessner A, Deneke B, Wörmann B

机构信息

Gerhard-Domagk-Institute of Pathology, University of Münster, Federal Republic of Germany.

出版信息

J Cancer Res Clin Oncol. 1992;118(5):349-60. doi: 10.1007/BF01294439.

Abstract

At clinical presentation, the majority of malignant tumors are composed of multiple clonal subpopulations of tumor cells with different phenotypic characteristics. Using the experimental tumor model ER 15-P, a methylcholanthrene-induced pleomorphic sarcoma of the C57 Bl6J mouse, we studied a system of long-term in vivo passages of this primary tumor for cell morphological changes, and alterations in the potential for spontaneous lung metastases. Transplants from the primary after the 4th, 20th, 40th and 80th i.m. passage (referred to as T4, T20, T40, and T80 respectively) together with their lung metastases were investigated by light microscopy, immunohistochemistry, and electron microscopy. In addition, the potential for metastasis to the lungs in each group was determined and compared with that of the parent T4 tumors. T4 tumors were mainly composed of spindle-shaped tumor cells with the ultrastructural features of fibroblasts and myofibroblasts, often arranged in a storiform or fasciculated growth pattern, and intermingled with tumor giant cells. Some small areas contained polygonal or rounded tumor cells, ultrastructurally undifferentiated, and sometimes arranged in a hemangiopericytoma-like growth pattern. Although electron-microscopical findings clearly demonstrated the mesenchymal origin of these tumor cells, immunostaining with a polyclonal antibody to vimentin was unspecific in all tumor cells and normal mouse tissue. Monoclonal antibodies to vimentin from different sources were completely negative in tumor cells and murine stromal components. In contrast, myofibroblast-like tumor cells showed immunohistochemically, a moderate to strong co-expression with monoclonal antibodies to desmin, muscle actin and alpha-smooth muscle actin. On the basis of these morphological findings, the primary ER 15-P was classified as a pleomorphic myofibrosarcoma. The lung metastases of T4 tumors were mainly composed of undifferentiated round to polygonal tumor cells, while the number of desmin-positive, muscle- and alpha-smooth muscle-actin-positive cells was reduced. The morphological features of T20 tumors and their lung metastases were the same as in T4, indicating a relative stability of the phenotype up to that stage. In contrast, T40 and T80 tumors and their lung metastases were found to contain almost exclusively undifferentiated tumor cells and many tumor giant cells. While fibroblast-like tumor cells were seen only occasionally, myofibroblast-like tumor cells had almost completely disappeared. The potential for lung metastases was nearly constant in all groups, suggesting metastatic stability. Obviously, the undifferentiated tumor cells of this model are associated with a higher metastatic potential.

摘要

在临床表现上,大多数恶性肿瘤是由具有不同表型特征的多种肿瘤细胞克隆亚群组成。我们使用实验性肿瘤模型ER 15-P(一种由甲基胆蒽诱导的C57 Bl6J小鼠多形性肉瘤),研究了该原发性肿瘤长期体内传代系统中细胞形态变化以及自发肺转移潜能的改变。对第4次、第20次、第40次和第80次肌肉注射传代后的原发性肿瘤移植瘤(分别称为T4、T20、T40和T80)及其肺转移灶进行了光学显微镜、免疫组织化学和电子显微镜检查。此外,测定了每组肿瘤的肺转移潜能,并与亲代T4肿瘤进行比较。T4肿瘤主要由梭形肿瘤细胞组成,具有成纤维细胞和肌成纤维细胞的超微结构特征,常呈车辐状或束状生长模式,并与肿瘤巨细胞混合存在。一些小区域含有多边形或圆形肿瘤细胞,超微结构未分化,有时呈血管外皮细胞瘤样生长模式。尽管电子显微镜检查结果清楚地表明这些肿瘤细胞起源于间充质,但用波形蛋白多克隆抗体进行免疫染色在所有肿瘤细胞和正常小鼠组织中均无特异性。来自不同来源的波形蛋白单克隆抗体在肿瘤细胞和小鼠基质成分中均完全阴性。相反,肌成纤维细胞样肿瘤细胞免疫组织化学显示,与结蛋白、肌动蛋白和α-平滑肌肌动蛋白单克隆抗体呈中度至强共表达。基于这些形态学发现,原发性ER 15-P被归类为多形性肌纤维肉瘤。T4肿瘤的肺转移灶主要由未分化的圆形至多边形肿瘤细胞组成,而结蛋白阳性、肌动蛋白和α-平滑肌肌动蛋白阳性细胞数量减少。T20肿瘤及其肺转移灶的形态特征与T4相同,表明直至该阶段表型相对稳定。相反,T40和T80肿瘤及其肺转移灶几乎完全由未分化肿瘤细胞和许多肿瘤巨细胞组成。仅偶尔可见成纤维细胞样肿瘤细胞,肌成纤维细胞样肿瘤细胞几乎完全消失。所有组的肺转移潜能几乎恒定,提示转移稳定性。显然,该模型中的未分化肿瘤细胞具有更高的转移潜能。

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