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Genetic alterations of RNA leukemia viruses associated with the development of spontaneous thymic leukemia in AKR/J mice.

机译:RNA白血病病毒的遗传改变与AKR / J小鼠自发性胸腺白血病的发展有关。

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摘要

T1-oligonucleotide fingerprinting and mapping were used to study the expression of RNA leukemia viruses in leukemic and preleukemic AKR/J mice, with techniques designed to minimize the loss or inadvertent selection of viruses in vitro before biochemical analysis. In leukemic animals, complex mixtures of ecotropic and mink-tropic viruses were expressed. Unique but similar polytropic virus-like genomes were present in each tumor isolate. In preleukemic mice, viral isolates from the thymus that were grown on NIH3T3 fibroblasts contained genomes with non-Akv polytropic virus-related oligonucleotides. This phenomenon was not evident in fingerprints of viruses from the spleen and bone marrow of the same animals. Remarkably, the non-Akv oligonucleotides located in the 3' portion of the P15E gene, the U3 noncoding region, and the 5' part of the gp70 gene were often expressed independently. Our results suggest the following. (i) Recombinant viruses can be detected in the thymuses of young preleukemic AKR mice and increase in relative abundance with age. (ii) During in vivo generation of the recombinant leukemogenic viruses, the selection of polytropic virus-related sequences in the 3' part of p15E and the U3 region and the 5' portion of gp70 occurs independently. (iii) Independent biological properties encoded in the gp70 and p15E regions of env of the recombinant viruses may mediate viral selection or leukemogenicity. (iv) The leukemogenic polytropic viruses of AKR/J mice arise via genetic recombination involving at least three endogenous viral sequences.
机译:T1寡核苷酸指纹图谱和作图被用于研究白血病和白血病前AKR / J小鼠中RNA白血病病毒的表达,并设计了旨在使生化分析之前体外病毒丢失或无意选择最小化的技术。在白血病动物中,表达了嗜性和貂性病毒的复杂混合物。每个肿瘤分离物中都存在独特但相似的多向病毒样基因组。在白血病前小鼠中,在NIH3T3成纤维细胞上生长的胸腺病毒分离株含有与非Akv多方病毒相关寡核苷酸的基因组。在同一动物的脾脏和骨髓的病毒指纹图中,这种现象并不明显。值得注意的是,位于P15E基因3'部分,U3非编码区和gp70基因5'部分的非Akv寡核苷酸通常独立表达。我们的结果表明以下几点。 (i)重组病毒可以在年轻的白血病前AKR小鼠的胸腺中检测到,并随着年龄的增长而相对增加。 (ii)在体内产生重组致白血病病毒期间,在p15E的3'部分和U3区域以及gp70的5'部分中多态病毒相关序列的选择独立发生。 (iii)重组病毒env的gp70和p15E区编码的独立生物学特性可能介导病毒选择或致白血病。 (iv)AKR / J小鼠的致白血病多方病毒是通过涉及至少三个内源性病毒序列的基因重组产生的。

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