Li Sheng-Fowler , Wei Tu , Kathryn Phy , Juliete Macauley , Lynda Lanning , Andrew M. Lewis Jr. , Keith Peden
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Tumors were induced in mice by pMSV-T24-H-<em>ras</em> plus pMSV-c-<em>myc</em> or by pMSV-T24-H-<em>ras</em>/MSV-c-<em>myc.</em> Because newborn hamsters and newborn rats have been recommended for oncogenicity testing of the DNA from tumorigenic mammalian cell-substrates used for vaccine production, we evaluated their sensitivity. Newborn hamsters and rats were inoculated with different doses of pMSV-T24-H-<em>ras</em>/MSV-c-<em>myc</em> to determine their sensitivity to tumor induction and with the single-oncogene-expression plasmids to determine whether single oncogenes could induce tumors. Newborn rats were more sensitive than newborn hamsters, and activated H-<em>ras</em> but not c-<em>myc</em> induced tumors in newborns of both rodent species. DNA from four cell lines established from tumors induced by pMSV-T24-H-<em>ras</em>/MSV-c-<em>myc</em> was inoculated into newborn rats. 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引用次数: 0
摘要
为了评估在致瘤细胞系中生产的疫苗中残留细胞DNA的风险,我们已经建立了体内试验来量化DNA的致癌活性。我们已经生成了三个癌基因表达质粒:表达活化的H-ras的pMSV-T24-H-ras;pMSV-c-myc,表达c-myc;以及表达两种致癌基因的pmv - t24 - h -ras/MSV-c-myc。pMSV-T24-H-ras加pMSV-c-myc或pMSV-T24-H-ras/MSV-c-myc在小鼠中诱导肿瘤。由于新生仓鼠和新生大鼠被推荐用于疫苗生产的致瘤性哺乳动物细胞底物DNA的致瘤性测试,我们评估了它们的敏感性。用不同剂量的pMSV-T24-H-ras/MSV-c-myc接种新生仓鼠和大鼠,测定其对肿瘤诱导的敏感性;用单癌基因表达质粒接种新生仓鼠和大鼠,测定单癌基因是否能诱导肿瘤。新生大鼠比新生仓鼠更敏感,在两种啮齿类动物的新生儿中激活了H-ras而不是c-myc诱导的肿瘤。将pmv - t24 - h -ras/MSV-c-myc诱导的肿瘤细胞系的DNA接种于新生大鼠。由于这种细胞DNA没有诱导肿瘤,这应该是最佳的,因为它包含连接的癌基因并存在于几个拷贝中,我们得出结论,现有的体内模型不够敏感,无法检测细胞DNA的致癌性。
Evaluating the sensitivity of newborn rats and newborn hamsters to oncogenic DNA
To evaluate the risk of residual cellular DNA in vaccines manufactured in tumorigenic cell lines, we have been establishing in vivo assays to quantify the oncogenic activity of DNA. We had generated three oncogene-expression plasmids: pMSV-T24-H-ras, which expresses activated H-ras; pMSV-c-myc, which expresses c-myc; and pMSV-T24-H-ras/MSV-c-myc, which expresses both oncogenes. Tumors were induced in mice by pMSV-T24-H-ras plus pMSV-c-myc or by pMSV-T24-H-ras/MSV-c-myc. Because newborn hamsters and newborn rats have been recommended for oncogenicity testing of the DNA from tumorigenic mammalian cell-substrates used for vaccine production, we evaluated their sensitivity. Newborn hamsters and rats were inoculated with different doses of pMSV-T24-H-ras/MSV-c-myc to determine their sensitivity to tumor induction and with the single-oncogene-expression plasmids to determine whether single oncogenes could induce tumors. Newborn rats were more sensitive than newborn hamsters, and activated H-ras but not c-myc induced tumors in newborns of both rodent species. DNA from four cell lines established from tumors induced by pMSV-T24-H-ras/MSV-c-myc was inoculated into newborn rats. Because no tumors were induced by this cellular DNA, which should be optimal as it contains both oncogenes linked and present in several copies, we conclude that available in vivo models are not sensitive enough to detect the oncogenicity of cellular DNA.
期刊介绍:
Accounts of Chemical Research presents short, concise and critical articles offering easy-to-read overviews of basic research and applications in all areas of chemistry and biochemistry. These short reviews focus on research from the author’s own laboratory and are designed to teach the reader about a research project. In addition, Accounts of Chemical Research publishes commentaries that give an informed opinion on a current research problem. Special Issues online are devoted to a single topic of unusual activity and significance.
Accounts of Chemical Research replaces the traditional article abstract with an article "Conspectus." These entries synopsize the research affording the reader a closer look at the content and significance of an article. Through this provision of a more detailed description of the article contents, the Conspectus enhances the article's discoverability by search engines and the exposure for the research.