首页> 美国卫生研究院文献>Journal of Virology >Ability of a T-antigen transport-defective mutant of simian virus 40 to immortalize primary cells and to complement polyomavirus middle T in tumorigenesis.

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Ability of a T-antigen transport-defective mutant of simian virus 40 to immortalize primary cells and to complement polyomavirus middle T in tumorigenesis.

机译：猿猴病毒40的T抗原转运缺陷型突变体永生原代细胞并在肿瘤发生过程中补充多瘤病毒中间T的能力。

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摘要

The oncogenic potential of polyomavirus in newborn rats could not be expressed by a genome encoding only the middle T antigen but required the presence of one of the other two viral early genes, small T or large T. The tumorigenicity defect could also be complemented by other viral or cellular genes that are known to be implicated in immortalization and establishment functions. The simian virus 40(cT)-3 mutant (R. E. Lanford and J. S. Butel, Cell 37:801-813, 1984), which fails to localize to the nucleus, has the capacity to complement polyomavirus middle T in tumorigenesis and to immortalize primary rat embryo fibroblasts when it was cotransfected in the presence of pSV2-neo. Our data suggested that under the conditions of DNA-mediated tumor induction and cotransfection with a dominant selection marker, the cellular alterations achieved by nonnuclear oncogenes such as polyomavirus small T and simian virus 40(cT)-3 were sufficient to complement polyomavirus middle T in transformation and tumorigenesis.

机译：多瘤病毒在新生大鼠中的致癌潜力不能通过仅编码中间T抗原的基因组来表达，而是需要存在另外两个病毒早期基因之一，即小T或大T。致瘤性缺陷也可以由其他已知与永生化和建立功能有关的病毒或细胞基因。猿猴病毒40（cT）-3突变体（RE Lanford和JS Butel，Cell 37：801-813，1984）无法定位到细胞核，具有在肿瘤发生过程中补充多瘤病毒中T并永生永生大鼠的能力。胚胎成纤维细胞在pSV2-neo存在下共转染。我们的数据表明，在DNA介导的肿瘤诱导和与显性选择标记共转染的条件下，由非核癌基因（如多瘤病毒小T和猿猴病毒40（cT）-3）实现的细胞改变足以补充多瘤病毒中T。转化和肿瘤发生。

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期刊名称 Journal of Virology
作者
J Vass-Marengo; A Ratiarson; C Asselin; M Bastin;
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年(卷),期 1986(59),3
年度 1986
页码 655–659
总页数 5
原文格式 PDF
正文语种
中图分类人体病毒学（致病病毒）;病毒（滤过性病毒）;
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入库时间 2022-08-17 11:45:07

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1. Ability of a T-antigen transport-defective mutant of simian virus 40 to immortalize primary cells and to complement polyomavirus middle T in tumorigenesis. [J] . J Vass-Marengo, A Ratiarson, C Asselin, Journal of Virology . 1986,第3期

机译：猿猴病毒40的T-抗原输送缺陷突变体的能力，使原发性细胞化并补充肿瘤内瘤中的多瘤血清T.
2. Ability of a T-antigen transport-defective mutant of simian virus 40 to immortalize primary cells and to complement polyomavirus middle T in tumorigenesis. [J] . J Vass-Marengo, A Ratiarson, C Asselin, Journal of Virology . 1986,第3期

机译：猿猴病毒40的T-抗原输送缺陷突变体的能力，使原发性细胞化并补充肿瘤内瘤中的多瘤血清T.
3. Ability of a T-antigen transport-defective mutant of simian virus 40 to immortalize primary cells and to complement polyomavirus middle T in tumorigenesis. [J] . J Vass-Marengo, A Ratiarson, C Asselin, Journal of Virology . 1986,第期

机译：猿猴病毒40的T-抗原输送缺陷突变体的能力，使原发性细胞化并补充肿瘤内瘤中的多瘤血清T.
4. Mutational analysis of the origin binding domain of simian virus 40 large T-antigen provides insights into its function in DNA unwinding. [D] . Foster, Erin C. 2010

机译：猿猴病毒40大T抗原的起源结合域的突变分析提供了对其在DNA解链中功能的了解。
5. Differential ability of a T-antigen transport-defective mutant of simian virus 40 to transform primary and established rodent cells. [O] . R E Lanford, C Wong, J S Butel 1985

机译：猿猴病毒40的T抗原转运缺陷型突变体转化原代和成熟啮齿动物细胞的差异能力。
6. Ability of a T-antigen transport-defective mutant of simian virus 40 to immortalize primary cells and to complement polyomavirus middle T in tumorigenesis [O] . J Vass-Marengo, A Ratiarson, C Asselin, 1986

机译：Simian病毒40的T-抗原传输缺陷突变体的能力，使原代细胞永生化并在肿瘤发生中补充多瘤中间T.

Ability of a T-antigen transport-defective mutant of simian virus 40 to immortalize primary cells and to complement polyomavirus middle T in tumorigenesis.

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