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通过核苷酸测序和异源双链分析对骨髓增殖性肉瘤病毒与莫洛尼鼠肉瘤病毒变体进行比较。

Comparison of myeloproliferative sarcoma virus with Moloney murine sarcoma virus variants by nucleotide sequencing and heteroduplex analysis.

作者信息

Stacey A, Arbuthnott C, Kollek R, Coggins L, Ostertag W

出版信息

J Virol. 1984 Jun;50(3):725-32. doi: 10.1128/JVI.50.3.725-732.1984.

Abstract

The myeloproliferative sarcoma virus (MPSV) was derived by passage of Moloney sarcoma virus (Mo-MuSV) in adult mice. Mo-MuSV variants transform fibroblasts. However, MPSV also affects erythroid, myeloid, and hematopoietic stem cells. The MPSV proviral genome, two temperature-sensitive mutants derived from it, Mo-MuSV variant M1, and Moloney murine leukemia virus (Mo-MuLV) were compared by heteroduplex mapping. MPSV wild type was found to have 1 kilobase pair deleted from the pol gene and to contain v-mos-related sequences. The 3' end of MPSV, including the oncogene-helper junctions, the v-mos gene, and the 3' long terminal repeat, was sequenced and compared with sequences of Mo-MuLV, MSV-124, and the mouse oncogene c-mos. From these data, MPSV appears to be either closely related to the original Mo-MuSV or an independent recombinant of Mo-MuLV and c-mos. Five possible explanations of the altered specificity of MPSV are considered. (i) The MPSV mos protein has properties inherent in c-mos but lost by other Mo-MuSV mos proteins. (ii) The MPSV mos protein has altered characteristics due to amino acid changes. (iii) Due to a frameshift, MPSV codes for a mos protein truncated at the amino terminal and also a novel peptide. (iv) A second novel peptide may be encoded from the 3' env region. (v) MPSV has long terminal repeats and an enhancer sequence more like Mo-MuLV than Mo-MuSV, with a consequently altered target cell specificity.

摘要

骨髓增殖性肉瘤病毒(MPSV)是通过莫洛尼肉瘤病毒(Mo-MuSV)在成年小鼠体内传代而获得的。Mo-MuSV变体可转化成纤维细胞。然而,MPSV也会影响红系、髓系和造血干细胞。通过异源双链图谱分析比较了MPSV前病毒基因组、由其衍生的两个温度敏感突变体、Mo-MuSV变体M1和莫洛尼鼠白血病病毒(Mo-MuLV)。发现MPSV野生型的pol基因缺失了1千碱基对,并含有与v-mos相关的序列。对MPSV的3'端,包括癌基因-辅助连接区、v-mos基因和3'长末端重复序列进行了测序,并与Mo-MuLV、MSV-124和小鼠癌基因c-mos的序列进行了比较。根据这些数据,MPSV似乎要么与原始的Mo-MuSV密切相关,要么是Mo-MuLV和c-mos的独立重组体。考虑了MPSV特异性改变的五种可能解释。(i)MPSV的mos蛋白具有c-mos固有的特性,但其他Mo-MuSV的mos蛋白已丧失这些特性。(ii)由于氨基酸变化,MPSV的mos蛋白具有改变的特性。(iii)由于移码,MPSV编码一个在氨基末端截短的mos蛋白以及一个新的肽段。(iv)可能从3' env区域编码第二个新的肽段。(v)MPSV的长末端重复序列和增强子序列更类似于Mo-MuLV而不是Mo-MuSV,因此其靶细胞特异性发生了改变。

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