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含有BK病毒早期区域和激活的人c-Harvey-ras癌基因的重组DNA在仓鼠中诱发恶性皮下肉瘤

Induction of malignant subcutaneous sarcomas in hamsters by a recombinant DNA containing BK virus early region and the activated human c-Harvey-ras oncogene.

作者信息

Corallini A, Pagnani M, Viadana P, Camellin P, Caputo A, Reschiglian P, Rossi S, Altavilla G, Selvatici R, Barbanti-Brodano G

机构信息

Institute of Microbiology, School of Medicine, University of Ferrara, Italy.

出版信息

Cancer Res. 1987 Dec 15;47(24 Pt 1):6671-7.

PMID:2824040
Abstract

Malignant undifferentiated sarcomas were induced in 11 of 15 (73.3%) newborn Syrian hamsters by s.c. inoculation of a recombinant DNA (pBK/c-rasA) containing BK virus (BKV) early region gene and the activated human c-Harvey-ras(c-Ha-ras) oncogene derived from T24 bladder carcinoma. The two genes inoculated independently as well as a recombinant DNA of BKV early region gene and normal human c-Ha-ras proto-oncogene were not tumorigenic. Tumor-derived cell lines propagated in culture were immortalized and had growth characteristics consistent with a fully transformed phenotype. Tumors and tumor cell lines showed tandem insertions of pBK/c-rasA in high copy number and expressed BKV- and c-Ha-ras-specific transcripts as well as BKV T-antigen and c-Ha-ras protein with a molecular weight of 21,000. We conclude that BKV DNA requires interaction with other oncogenic functions for tumorigenicity. These findings may be relevant to the role of BKV in human neoplasia, where cooperation or synergism between BKV and cellular oncogenes could occur as an aspect of the multifactorial process of carcinogenesis.

摘要

通过皮下接种含有BK病毒(BKV)早期区域基因和源自T24膀胱癌的活化人c-Harvey-ras(c-Ha-ras)癌基因的重组DNA(pBK/c-rasA),在15只新生叙利亚仓鼠中的11只(73.3%)诱发了恶性未分化肉瘤。单独接种的这两个基因以及BKV早期区域基因与正常人c-Ha-ras原癌基因的重组DNA均无致瘤性。在培养中传代的肿瘤衍生细胞系永生化,具有与完全转化表型一致的生长特性。肿瘤和肿瘤细胞系显示pBK/c-rasA以高拷贝数串联插入,并表达BKV和c-Ha-ras特异性转录本以及BKV T抗原和分子量为21,000的c-Ha-ras蛋白。我们得出结论,BKV DNA需要与其他致癌功能相互作用才能具有致瘤性。这些发现可能与BKV在人类肿瘤形成中的作用相关,在人类肿瘤形成中,BKV与细胞癌基因之间的合作或协同作用可能作为致癌多因素过程的一个方面而发生。

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