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首页> 外文期刊>British Journal of Cancer >Murine melanoma: a model for intracranial metastasis
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Murine melanoma: a model for intracranial metastasis

机译:小鼠黑色素瘤:颅内转移的模型。

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A variant subline (B16-F10-B2) selected from the B16-F10 melanoma cell line, shows greater metastatic capacity and preferential growth in the brain after i.v. injection into C57BL/6 mice. Several biological properties of these two cell lines have been compared, in an effort to determine the mechanisms responsible for this non-random metastatic pattern. No differences in cell morphology, in vitro growth rates or exposed cell-surface proteins were detected. Quantitative analysis of tumour-cell arrest and distribution using 125IUdR-labelled cells indicated that, although initial arrest patterns of the cell lines were very similar, B16-F10-B2 cells survived in the lungs to a greater cell line had a higher mean number of chromosomes than the parent line, whereas the variance of chromosome distribution was less. We suggest that the selection of a brain-colonizing variant represents the emergence of a pre-existing subpopulation of cells, and provides a useful model for studying mechanisms of intracranial metastasis.
机译:选自B16-F10黑色素瘤细胞系的变体亚系(B16-F10-B2)在静脉注射后显示出更高的转移能力并在大脑中优先生长。注射到C57BL / 6小鼠中。为了确定造成这种非随机转移模式的机制,已经比较了这两种细胞系的几种生物学特性。没有检测到细胞形态,体外生长速率或暴露的细胞表面蛋白差异。使用125IUdR标记的细胞对肿瘤细胞的阻滞和分布进行定量分析表明,尽管细胞系的初始阻滞模式非常相似,但B16-F10-B2细胞在肺中存活,而更大的细胞系具有更高的平均数。染色体比亲本染色体少,而染色体分布的变异少。我们建议,选择一个脑部殖民化的变种代表一个预先存在的细胞亚群的出现,并为研究颅内转移的机制提供有用的模型。

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