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人类结肠癌恶性细胞的异质性。

Heterogeneity of malignant cells from a human colonic carcinoma.

作者信息

Brattain M G, Fine W D, Khaled F M, Thompson J, Brattain D E

出版信息

Cancer Res. 1981 May;41(5):1751-6.

PMID:7214343
Abstract

Three subpopulations of malignant cells were isolated from a primary cell culture of a single human colonic carcinoma. The variant cells were established as cell lines designated HCT 116, HCT 116a, and HCT 116b, respectively. In vitro characterizations of the variant lines included growth in 0.5% agarose and growth on confluent layers of mouse fibroblasts. HCT 116a showed the highest colony formation in agarose and on confluent fibroblasts, while colony formation by HCT 116 was higher than that of HCT 116b in both of these systems. All of the variant lines were tumorigenic in athymic nude mice given injections of 10 x 10(6) cells, but the time between inoculation and tumor development (latency period) was approximately 10 times longer for HCT 116b as for HCT 116a and 8 times longer than for HCT 116. HCT 116b was not tumorigenic at an inoculum of 5 x 10(6) cells, while both HCT 116 and 116a were tumorgenic at this level. However, HCT 116a was clearly more tumorigenic than was HCT 116 on the basis of the number of animals developing tumors at inoculate of both 10 x 10(6) and 5 x 10(6) cells and on the basis of their differences in latency periods. While all the cell lines had near diploid numbers of chromosomes, each line showed a distinct histological pattern when grown as xenografts in athymic nude mice.

摘要

从一名人类结肠癌患者的原代细胞培养物中分离出了三个恶性细胞亚群。这些变异细胞分别被建立为命名为HCT 116、HCT 116a和HCT 116b的细胞系。对这些变异细胞系的体外特性分析包括在0.5%琼脂糖中的生长情况以及在汇合的小鼠成纤维细胞层上的生长情况。HCT 116a在琼脂糖中和汇合的成纤维细胞上显示出最高的集落形成能力,而在这两个系统中,HCT 116的集落形成能力均高于HCT 116b。给无胸腺裸鼠注射10×10(6)个细胞时,所有变异细胞系都具有致瘤性,但HCT 116b从接种到肿瘤形成的时间(潜伏期)大约是HCT 116a 的10倍,是HCT 116的8倍。接种5×10(6)个细胞时,HCT 116b没有致瘤性,而HCT 116和116a在此接种水平下具有致瘤性。然而,基于接种10×10(6)个细胞和5×10(6)个细胞时发生肿瘤的动物数量以及潜伏期的差异,HCT 116a的致瘤性明显高于HCT 116。虽然所有细胞系的染色体数目接近二倍体,但当作为异种移植物在无胸腺裸鼠体内生长时,每个细胞系都呈现出独特的组织学模式。

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