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一个活化的人类c-raf-1基因的分子克隆与特性分析

Molecular cloning and characterization of an activated human c-raf-1 gene.

作者信息

Fukui M, Yamamoto T, Kawai S, Mitsunobu F, Toyoshima K

出版信息

Mol Cell Biol. 1987 May;7(5):1776-81. doi: 10.1128/mcb.7.5.1776-1781.1987.

Abstract

Results of previous studies have shown that a raf-related transforming DNA sequence is present in NIH 3T3 transformants that are derived from GL-5-JCK human glioblastoma DNA transfection. The transforming DNA was molecularly cloned by using cosmid vector pJB8 to determine its structure and origin. Analyses of selected clones revealed that the transforming DNA consisted of three portions of human DNA sequences, with the 3' half of the c-raf-1 gene as its middle portion. This raf region was about 20 kilobases long and contained exons 8 to 17 and the poly(A) addition site. RNA blot analysis showed that the raf-related transforming DNA was transcribed into 5.3-, 4.8-, and 2.5-kilobase mRNAs; the 2.5-kilobase transcript was thought to be the major transcript. Immunoprecipitation analyses revealed that a 44-kilodalton raf-related protein was specifically expressed in the NIH 3T3 transformants. The raf-related transforming DNA was considered to be activated when its amino-terminal sequence was truncated and the DNA was coupled with a foreign promoter sequence. On hybridization analysis of the original GL-5-JCK glioblastoma DNA, no rearrangement of c-raf-1 was detectable in the tumor DNA. The rearrangement of c-raf-1 may have occurred during transfection or may have been present in a small population of the original tumor cells as a result of tumor progression.

摘要

先前的研究结果表明,在源自GL-5-JCK人胶质母细胞瘤DNA转染的NIH 3T3转化体中存在一种与raf相关的转化DNA序列。通过使用粘粒载体pJB8对转化DNA进行分子克隆,以确定其结构和来源。对选定克隆的分析表明,转化DNA由三部分人类DNA序列组成,其中间部分为c-raf-1基因的3'半段。这个raf区域约20千碱基长,包含外显子8至17以及聚腺苷酸添加位点。RNA印迹分析表明,与raf相关的转化DNA被转录为5.3、4.8和2.5千碱基的mRNA;2.5千碱基的转录本被认为是主要转录本。免疫沉淀分析表明,一种44千道尔顿的与raf相关的蛋白质在NIH 3T3转化体中特异性表达。当与raf相关的转化DNA的氨基末端序列被截短且DNA与外源启动子序列偶联时,该转化DNA被认为是活化的。对原始GL-5-JCK胶质母细胞瘤DNA进行杂交分析时,在肿瘤DNA中未检测到c-raf-1的重排。c-raf-1的重排可能发生在转染过程中,或者可能由于肿瘤进展而存在于原始肿瘤细胞的一小部分中。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f81f/365279/12361cf0fe7f/molcellb00077-0206-a.jpg

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