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新型DNA重排与二氢叶酸还原酶基因扩增相关。

Novel DNA rearrangements are associated with dihydrofolate reductase gene amplification.

作者信息

Federspiel N A, Beverley S M, Schilling J W, Schimke R T

出版信息

J Biol Chem. 1984 Jul 25;259(14):9127-40.

PMID:6086622
Abstract

We have employed the technique of chromosome "walking" to determine the structure of 240 kilobases of amplified DNA surrounding the dihydrofolate reductase gene in methotrexate-resistant mouse cell lines. Within this region, we have found numerous DNA rearrangements which occurred during the amplification process. DNA subclones from regions flanking the dihydrofolate reductase gene were also utilized as hybridization probes in other cell lines. Our results show that: 1) amplification-specific DNA rearrangements or junctions are unique to each cell line; 2) within a given cell line, multiple amplification-specific DNA sequence rearrangements are found; 3) the degree of amplification of sequences flanking the dihydrofolate reductase gene shows quantitative variation among and within cell lines; and 4) both the arrangement of amplified sequences as well as the magnitude of gene amplification may vary with prolonged culture even under maintenance selection conditions. These studies indicate that there is no static repetitive unit amplified in these cells. Rather, a dynamic and complex arrangement of the amplified sequences exists which is continually changing.

摘要

我们运用染色体“步移”技术来确定甲氨蝶呤抗性小鼠细胞系中二氢叶酸还原酶基因周围240千碱基对扩增DNA的结构。在该区域内,我们发现了许多在扩增过程中发生的DNA重排。来自二氢叶酸还原酶基因侧翼区域的DNA亚克隆也被用作其他细胞系中的杂交探针。我们的结果表明:1)扩增特异性DNA重排或连接对于每个细胞系都是独特的;2)在给定的细胞系中,发现了多个扩增特异性DNA序列重排;3)二氢叶酸还原酶基因侧翼序列的扩增程度在细胞系之间和细胞系内部显示出定量变化;4)即使在维持选择条件下,随着培养时间的延长,扩增序列的排列以及基因扩增的幅度都可能发生变化。这些研究表明,在这些细胞中不存在静态的重复扩增单元。相反,存在一种动态且复杂的扩增序列排列,并且这种排列在不断变化。

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