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通过一种新方法在禽肾母细胞瘤中鉴定出一种前病毒激活的c-Ha-ras癌基因:一种嵌合病毒-宿主转录本的cDNA克隆

Identification of a provirally activated c-Ha-ras oncogene in an avian nephroblastoma via a novel procedure: cDNA cloning of a chimaeric viral-host transcript.

作者信息

Westaway D, Papkoff J, Moscovici C, Varmus H E

出版信息

EMBO J. 1986 Feb;5(2):301-9. doi: 10.1002/j.1460-2075.1986.tb04213.x.

Abstract

Retrovirus without oncogenes often exert their neoplastic potential as insertional mutagens of cellular proto-oncogenes. This may be associated with the production of chimaeric viral-host transcripts; in these cases; activated cellular genes can be identified by obtaining cDNA clones of bipartite RNAs. This approach was used in the analysis of chicken nephroblastomas induced by myeloblastosis-associated virus (MAV). One tumor contained a novel mRNA species initiated within a MAV LTR. cDNA cloning revealed that this mRNA encodes a protein of 189 amino acids, identical to that of normal human Ha-ras-1 at 185 positions, including positions implicated in oncogenic activation of ras proto-oncogenes; there are no differences between the coding sequences of presumably normal Ha-ras cDNA clones from chicken lymphoma RNA and the tumor-derived cDNAs. The chimaeric mRNA in the nephroblastoma is at least 25-fold more abundant than c-Ha-ras mRNA in normal kidney tissue, and a 21-kd ras-related protein is present in relatively large amounts in the tumor. We conclude that a quantitative change in c-Ha-ras gene expression results from an upstream insertion mutation and presumably contributes to tumorigenesis in this single case. Little or no increase in c-Ha-ras RNA or protein was observed in other nephroblastomas.

摘要

不含癌基因的逆转录病毒常作为细胞原癌基因的插入诱变剂发挥其致瘤潜能。这可能与嵌合病毒 - 宿主转录本的产生有关;在这些情况下,可通过获得二分体RNA的cDNA克隆来鉴定活化的细胞基因。该方法用于分析成髓细胞增多症相关病毒(MAV)诱导的鸡肾母细胞瘤。一个肿瘤含有一种在MAV长末端重复序列(LTR)内起始的新型mRNA。cDNA克隆显示该mRNA编码一种189个氨基酸的蛋白质,在185个位置与正常人Ha-ras-1相同,包括与ras原癌基因致癌激活有关的位置;来自鸡淋巴瘤RNA的推测正常的Ha-ras cDNA克隆与肿瘤来源的cDNA的编码序列之间没有差异。肾母细胞瘤中的嵌合mRNA比正常肾组织中的c-Ha-ras mRNA丰富至少25倍,并且肿瘤中相对大量存在一种21kd的ras相关蛋白。我们得出结论,c-Ha-ras基因表达的定量变化是由上游插入突变引起的,并且在这一单一病例中可能促成肿瘤发生。在其他肾母细胞瘤中未观察到c-Ha-ras RNA或蛋白质有很少增加或没有增加。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5405/1166733/da16dabe1fe2/emboj00165-0097-a.jpg

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