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MOPC 21小鼠骨髓瘤细胞系中重排的c-mos基因座及其在杂交瘤中的持续性。

Rearranged c-mos locus in a MOPC 21 murine myeloma cell line and its persistence in hybridomas.

作者信息

Gattoni-Celli S, Hsiao W L, Weinstein I B

出版信息

Nature. 1983;306(5945):795-6. doi: 10.1038/306795a0.

Abstract

Studies of a number of normal and carcinogen-transformed murine cell lines, and a variety of murine tissues, have indicated that, in contrast to several other cellular oncogenes, the oncogene c-mos gene is usually transcriptionally silent. The recent report by Rechavi et al. indicating that in the mouse myeloma XRPC24 originally induced by pristane (2,6,10-14-tetramethylpentadecane) the c-mos gene is rearranged and transcriptionally active, and that it can transform murine fibroblasts in a transfection assay, is therefore of considerable interest. Here we show that the c-mos locus has undergone a similar rearrangement, and is also transcriptionally active, in the cell line P3-X63-Ag8-653, a derivative of the mouse myeloma MOPC 21 which was induced by mineral oil. This line is widely used for making hybridomas that synthesize monoclonal antibodies. We also demonstrate that the rearranged c-mos sequence is maintained in three different hybridomas derived by fusion of this cell line with normal murine spleen lymphocytes, suggesting that it may play a role in the continuous growth and/or constitutive immunoglobulin production by these hybridomas.

摘要

对一些正常的和经致癌物转化的鼠细胞系以及多种鼠组织的研究表明,与其他几种细胞癌基因不同,癌基因c-mos基因通常在转录上是沉默的。Rechavi等人最近的报告指出,在最初由 pristane(2,6,10 - 14 - 四甲基十五烷)诱导的小鼠骨髓瘤XRPC24中,c-mos基因发生了重排且转录活跃,并且在转染实验中它能转化鼠成纤维细胞,因此这一发现备受关注。在此我们表明,在细胞系P3-X63-Ag8-653中,c-mos基因座也经历了类似的重排,并且转录活跃,该细胞系是由矿物油诱导的小鼠骨髓瘤MOPC 21的衍生物。此细胞系被广泛用于制备合成单克隆抗体的杂交瘤。我们还证明,通过将该细胞系与正常鼠脾淋巴细胞融合得到的三种不同杂交瘤中均保留了重排的c-mos序列,这表明它可能在这些杂交瘤的持续生长和/或组成型免疫球蛋白产生中发挥作用。

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