化学致癌物对人淋巴母细胞样细胞系的超转化。

D Le François-Chabas, L Montagnier
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摘要

我们研究了遗传、病毒和诱变因素共同作用下人淋巴样细胞的体外恶性进展。采用Epstein-Barr病毒永生化淋巴母细胞系;它来自一位患有共济失调毛细血管扩张症的患者,这是一种与DNA修复缺陷有关的遗传性疾病。细胞被亚毒性剂量的两种强效诱变剂(致癌物)NQO(4-硝基喹啉-氧化物)和r7000(2-硝基-7-甲氧基-萘-呋喃)处理。处理后的细胞在软琼脂糖中形成集落的能力增强,其中出现了一些致密的集落,与未处理的对照细胞形成的弥漫性集落不同。从这些致密菌落衍生出的亚克隆与原始细胞的不同之处在于它们在液体培养基中的表现,它们在裸鼠中的致瘤性增加,以及它们在鸡绒毛膜上形成结节的能力。一些亚克隆在裸鼠中产生非退行性大肿瘤,其细胞接种量低于伯基特淋巴瘤细胞所需的细胞接种量,而侵入性低于后者。然而,从形态上看,亚克隆的恶性细胞与原始的淋巴母细胞样细胞相似。因此,在体外获得的这种恶性进展不能被认为与导致非洲儿童伯基特淋巴瘤的恶性进展相同。
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[Supertransformation of a human lymphoblastoid cell line by chemical carcinogens].

We have studied the in vitro malignant progression of human lymphoid cells by the combined effect of genetic, viral and mutagenic factors. A lymphoblastoid cell line immortalized by Epstein-Barr virus was used; it was derived from a patient suffering from ataxia-telangiectasia, a genetic disease linked to a deficiency in DNA repair. Cells were treated by sub-toxic doses of two potent mutagens (carcinogens), NQO (4-nitroquinolein-oxid) and R 7 000 (2-nitro-7-methoxy-naphto-furan). The treated cells showed an increased ability to form colonies in soft agarose, among which some compact colonies appeared, different from the diffuse colonies formed by untreated control cells. Sub-clones derived from these compact colonies differ also from the original cells by their behavior in liquid culture medium, by their increased tumorigenicity in Nude Mice and by their capacity to form nodules on Chicken chorioallantoic membrane. Some of the sub-clones produce non-regressing large tumors in Nude Mice with a cell inoculum lower than that required for Burkitt lymphoma cells while being less invasive than the latter. However, by their morphology, the malignant cells of the sub-clones remain similar to the original lymphoblastoid cells. Thus, such a malignant progression obtained in vitro cannot be considered as identical to that which leads to Burkitt lymphoma in African children.

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