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癌基因与辐射及病毒诱导的小鼠骨肉瘤的关系。

Oncogene involvement in radiation- and virus-induced mouse osteosarcomas.

作者信息

Merregaert J, Michiels L, van der Rauwelaert E, Lommel M, Gol-Winkler R, Janowski M

出版信息

Leuk Res. 1986;10(7):915-21. doi: 10.1016/0145-2126(86)90323-1.

DOI:10.1016/0145-2126(86)90323-1
PMID:3016418
Abstract

Internal irradiation of mice using bone seeking radionuclides results in the activation of endogenous retroviruses and in the subsequent development of bone tumors. Genomic DNA from an osteosarcoma cell line, derived from an 90Sr-induced bone tumor, was cotransfected with the plasmid pSV2-neo into NIH/3T3 cells and G418-resistant transfectants gave rise to colonies in soft agar. Southern blot analysis of these first cycle transformants revealed the presence of extra copies of c-ras. We have analysed the arrangement of ecotropic murine leukemia proviral sequences in seven 90Sr-induced bone tumors and one osteosarcoma cell line of CF1-mice. Integration of ecotropic and/or ecotropic recombinant proviruses seems to be involved in rearrangements of 3' provirus cellular junction fragments occurring in all tumor DNAs analysed, but no indication for site-specific integration was found. We also determined the primary structure of FBR-MuSV, a transforming retrovirus able to induce bone tumors in newborn mice. FBR-MuSV contains sequences from all four exons of the murine c-fos gene, but lacks sequences encoding the first 24 and the last 98 amino acids of the c-fos gene product. The coding region of FBR-MuSV has also undergone two small in frame deletions. Thus, the v-fosFBR-MuSV retains 236 amino acids of the 380 amino acids of the murine c-fos product. In FBR-MuSV-transformed cells two fos-containing mRNAs have been detected: a 3.3-kb full-size genomic RNA and a 2.2-kb subgenomic mRNA as revealed by both fos- and MuLV-hybridization probes.

摘要

使用亲骨性放射性核素对小鼠进行体内照射会导致内源性逆转录病毒激活,并随后引发骨肿瘤。从锶 - 90诱导的骨肿瘤中获取的骨肉瘤细胞系的基因组DNA,与质粒pSV2 - neo共转染到NIH/3T3细胞中,对G418有抗性的转染子在软琼脂中形成菌落。对这些第一代转化体的Southern印迹分析显示存在额外拷贝的c - ras。我们分析了CF1小鼠的七个锶 - 90诱导的骨肿瘤和一个骨肉瘤细胞系中嗜亲性鼠白血病前病毒序列的排列。嗜亲性和/或嗜亲性重组前病毒的整合似乎参与了所有分析的肿瘤DNA中发生的3'前病毒细胞连接片段的重排,但未发现位点特异性整合的迹象。我们还确定了FBR - MuSV的一级结构,FBR - MuSV是一种能够在新生小鼠中诱导骨肿瘤的转化逆转录病毒。FBR - MuSV包含来自小鼠c - fos基因所有四个外显子的序列,但缺少编码c - fos基因产物前24个和最后98个氨基酸的序列。FBR - MuSV的编码区也经历了两个小的框内缺失。因此,v - fosFBR - MuSV保留了小鼠c - fos产物380个氨基酸中的236个氨基酸。在FBR - MuSV转化的细胞中检测到两种含fos的mRNA:一种3.3kb的全长基因组RNA和一种2.2kb的亚基因组mRNA,这是通过fos和MuLV杂交探针揭示的。

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Oncogene involvement in radiation- and virus-induced mouse osteosarcomas.癌基因与辐射及病毒诱导的小鼠骨肉瘤的关系。
Leuk Res. 1986;10(7):915-21. doi: 10.1016/0145-2126(86)90323-1.
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Characterization of the FBR-murine osteosarcoma virus complex: FBR-MuSV encodes a FOS-derived oncogene.FBR-小鼠骨肉瘤病毒复合体的特性:FBR-MuSV编码一种源自FOS的癌基因。
Int J Cancer. 1984 Apr 15;33(4):511-7. doi: 10.1002/ijc.2910330415.
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Genome organisation of the FBR-osteosarcoma virus complex: identification of a subgenomic fos-specific message.FBR-骨肉瘤病毒复合体的基因组组织:亚基因组fos特异性信息的鉴定。
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[Isolation and characterization of retroviruses expressed in murine osteosarcomas induced by 90Sr].[90锶诱导的小鼠骨肉瘤中表达的逆转录病毒的分离与鉴定]
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Detection and identification of activated oncogenes in human skin cancers occurring on sun-exposed body sites.对暴露于阳光下身体部位发生的人类皮肤癌中激活的致癌基因的检测与鉴定。
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Extended life span and tumorigenicity of nonestablished mouse connective tissue cells transformed by the fos oncogene of FBR-MuSV.FBR-MuSV的fos癌基因转化的未定型小鼠结缔组织细胞的寿命延长和致瘤性
Cell. 1985 Jun;41(2):629-37. doi: 10.1016/s0092-8674(85)80035-0.

引用本文的文献

1
Oncogenes and radiation carcinogenesis.癌基因与辐射致癌作用
Environ Health Perspect. 1991 Jun;93:45-9. doi: 10.1289/ehp.919345.