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通过计算机分析在真核生物DNA中鉴定出的高度重复序列元件通常与调控序列或蛋白质结合位点同源。

Highly recurring sequence elements identified in eukaryotic DNAs by computer analysis are often homologous to regulatory sequences or protein binding sites.

作者信息

Bodnar J W, Ward D C

出版信息

Nucleic Acids Res. 1987 Feb 25;15(4):1835-51. doi: 10.1093/nar/15.4.1835.

Abstract

We have used computer assisted dot matrix and oligonucleotide frequency analyses to identify highly recurring sequence elements of 7-11 base pairs in eukaryotic genes and viral DNAs. Such elements are found much more frequently than expected, often with an average spacing of a few hundred base pairs. Furthermore, the most abundant repetitive elements observed in the ovalbumin locus, the beta-globin gene cluster, the metallothionein gene and the viral genomes of SV40, polyoma, Herpes simplex-1 and Mouse Mammary Tumor Virus were sequences shown previously to be protein binding sites or sequences important for regulating gene expression. These sequences were present in both exons and introns as well as promoter regions. These observations suggest that such sequences are often highly overrepresented within the specific gene segments with which they are associated. Computer analysis of other genetic units, including viral genomes and oncogenes, has identified a number of highly recurring sequence elements that could serve similar regulatory or protein-binding functions. A model for the role of such reiterated sequence elements in DNA organization and function is presented.

摘要

我们利用计算机辅助点阵和寡核苷酸频率分析,来识别真核基因和病毒DNA中7至11个碱基对的高度重复序列元件。这类元件的出现频率比预期高得多,平均间距通常为几百个碱基对。此外,在卵清蛋白基因座、β-珠蛋白基因簇、金属硫蛋白基因以及SV40、多瘤病毒、单纯疱疹病毒1型和小鼠乳腺肿瘤病毒的病毒基因组中观察到的最丰富的重复元件,是先前已证明的蛋白质结合位点或对调节基因表达很重要的序列。这些序列存在于外显子、内含子以及启动子区域中。这些观察结果表明,这类序列在与其相关的特定基因片段中往往高度富集。对包括病毒基因组和癌基因在内的其他遗传单位的计算机分析,已经识别出许多可能具有类似调节或蛋白质结合功能的高度重复序列元件。本文提出了一个关于此类重复序列元件在DNA组织和功能中作用的模型。

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本文引用的文献

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Supercoiled loops and eucaryotic DNA replicaton.超螺旋环与真核生物DNA复制
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A fixed site of DNA replication in eucaryotic cells.真核细胞中DNA复制的固定位点。
Cell. 1980 Feb;19(2):527-36. doi: 10.1016/0092-8674(80)90527-9.
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