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通过v-myc、v-ras和v-raf使小鼠原代脾细胞永生化。

Immortalization of murine primary spleen cells by v-myc, v-ras, and v-raf.

作者信息

Darnbrough C, Slater S, Vass M, MacDonald C

机构信息

Department of Immunology, University of Strathclyde, Todd Centre, Glasgow, United Kingdom.

出版信息

Exp Cell Res. 1992 Aug;201(2):273-83. doi: 10.1016/0014-4827(92)90274-c.

Abstract

Growth factor-independent cell lines, including four lines characterized as macrophages, were isolated by infection of BALB/c mouse primary spleen cells with combinations of three retroviruses encoding v-myc, v-ras, and v-myc/v-raf. Proliferating cell lines were isolated only rarely, and after long crisis periods, following the introduction of myc and raf by infection with J2 virus, or of myc and ras by coinfection with myc309 and raszip6 viruses. However, sequential infections with all three viruses--myc plus ras cells reinfected with J2, or J2 followed by myc plus ras coinfection--resulted in rapid outgrowth of cell lines which grew at high growth rates to high densities. When cells were treated with anti-IgG F(ab')2/IL-4/IL-5 to specifically stimulate B cells, cell lines were isolated readily by infection with myc plus ras alone, J2 alone, or all three viruses. These cell lines arose after shorter crisis times and all grew at high growth rates and to high densities. Analysis of cell surface markers and immunoglobulin gene arrangement revealed no lymphoid characteristics in any of the lines. Four cell lines express all three macrophage markers analyzed (F4/80, Mac1, FcR), and many others are Mac1+ and/or FcR+. Out of 20 immortalized cell lines tested, 13 show clonal growth in soft agar, and 3/6 of these produced tumors in BALB/c mice, indicating that fully transformed cells may be isolated by these procedures. In at least one of the cell lines, integration of all three infecting viruses has occurred.

摘要

通过用编码v-myc、v-ras和v-myc/v-raf的三种逆转录病毒组合感染BALB/c小鼠原代脾细胞,分离出了不依赖生长因子的细胞系,其中包括四种被鉴定为巨噬细胞的细胞系。增殖细胞系分离得非常罕见,且是在经过长时间的危机期之后,通过用J2病毒感染导入myc和raf,或通过用myc309和raszip6病毒共感染导入myc和ras之后才得以分离。然而,用所有三种病毒进行连续感染——用J2再次感染myc加ras细胞,或先感染J2再进行myc加ras共感染——导致细胞系快速生长,这些细胞系以高生长速率生长至高密度。当用抗IgG F(ab')2/IL-4/IL-5处理细胞以特异性刺激B细胞时,仅通过用myc加ras单独感染、单独感染J2或用所有三种病毒感染就能轻易分离出细胞系。这些细胞系在较短的危机期后出现,且都以高生长速率生长至高密度。对细胞表面标志物和免疫球蛋白基因排列的分析表明,所有细胞系均无淋巴细胞特征。四个细胞系表达了所分析的所有三种巨噬细胞标志物(F4/80、Mac1、FcR),许多其他细胞系为Mac1+和/或FcR+。在测试的20个永生化细胞系中,有13个在软琼脂中呈克隆生长,其中3/6在BALB/c小鼠中产生肿瘤,这表明通过这些程序可以分离出完全转化的细胞。在至少一个细胞系中,所有三种感染病毒均已整合。

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