人类v- able细胞同源物。

N Heisterkamp, J Groffen, J R Stephenson
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引用次数: 0

摘要

从一个具有代表性的人肺癌DNA文库中分离出一个连续的细胞DNA序列区域,长度为64 kb,代表了三个独立的cosmid克隆重叠的细胞插入。在细胞基因组的这个区域内,v-abl同源序列分布在大约32 kb的总区域内。这些序列代表了整个v-abl人类细胞同源物,与病毒v-abl转化基因共线,并且包含至少7个中间序列。至少有8个高度重复的DNA序列区域被证明与c-abl编码序列非常接近。除了主要的c-abl人类位点外,人类DNA序列的三个区域仅对应于v-abl基因的部分,已被鉴定出来。其中两个已被分子克隆,并显示出不同于主要的人类c-abl位点。转染培养的大鼠胚胎成纤维细胞后,含有v-abl同源序列的cosmid dna均未表现出转化活性。这些发现确定并绘制了人类DNA的单一遗传位点c-abl,代表了完整的v-abl同源物,并证明存在与v-abl更有限的亚基因组区域相对应的其他人类DNA序列。
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The human v-abl cellular homologue.

A contiguous region of cellular DNA sequence, 64 kb in length and representing overlapping cellular inserts from three independent cosmid clones, has been isolated from a representative library of human lung carcinoma DNA partially digested with MboI. Within this region of the cellular genome, v-abl homologous sequences are dispersed over a total region of around 32 kb. These sequences represent the entire v-abl human cellular homologue, are colinear with the viral v-abl transforming gene, and contain a minimum of seven intervening sequences. At least eight regions of highly repetitive DNA sequences have been shown to map in close proximity to c-abl coding sequences. In addition to the major c-abl human locus, three regions of human DNA sequence, corresponding to only portions of the v-abl gene, have been identified. Two of these have been molecularly cloned and shown to be distinct from the primary human c-abl locus. Upon transfection to rat embryo fibroblasts in culture, none of the cosmid DNAs containing v-abl homologous sequences exhibited transforming activity. These findings identify and map a single genetic locus of human DNA, c-abl, representing the complete v-abl homologue, and demonstrate the existence of additional human DNA sequences corresponding to more limited, subgenomic regions of v-abl.

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