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哺乳动物细胞中转染的重复序列间的分子内重组是不保守的。

Intramolecular recombination between transfected repeated sequences in mammalian cells is nonconservative.

作者信息

Chakrabarti S, Seidman M M

出版信息

Mol Cell Biol. 1986 Jul;6(7):2520-6. doi: 10.1128/mcb.6.7.2520-2526.1986.

Abstract

When plasmids carrying a fragmented gene with segments present as direct repeats are introduced into mammalian cells, recombination or gene conversion between the repeated sequences can reconstruct the gene. Intramolecular recombination leads to the deletion of the intervening sequences and the loss of one copy of the repeat. This process is known to be stimulated by double-strand breaks. Two current models for recombination in eucaryotic cells propose that the reaction is initiated by double-strand breaks, but differ in their predictions as to the fate of the intervening sequences. One model suggests that these sequences are always lost, while the other indicates that the reaction will be conservative as a function of the position of the double-strand break. We have constructed a plasmid in which two overlapping portions of the simian virus 40 early region, which contains the origin and T-antigen gene, are present as direct repeats separated by sequences containing a plasmid with a simian virus 40 origin of replication. Recombination across the repeated segments could produce a plasmid with an origin of replication and/or a plasmid with a gene for a functional T-antigen which would drive the replication of both. Introduction of this construction into African green monkey kidney cells, without coinfection, establishes a condition in which the products of the recombination or gene conversion can be interpreted unambiguously. We find that the majority of the reconstruction reactions are nonconservative.

摘要

当携带一个断裂基因(其片段以直接重复序列形式存在)的质粒被导入哺乳动物细胞时,重复序列之间的重组或基因转换可以重建该基因。分子内重组会导致中间序列的缺失以及一个重复拷贝的丢失。已知这一过程会受到双链断裂的刺激。目前关于真核细胞重组的两种模型提出,反应由双链断裂引发,但在对中间序列命运的预测上存在差异。一种模型认为这些序列总是会丢失,而另一种模型则表明反应会根据双链断裂的位置而具有保守性。我们构建了一个质粒,其中猴病毒40早期区域的两个重叠部分(包含复制起点和T抗原基因)以直接重复序列形式存在,中间被一段包含带有猴病毒40复制起点的质粒的序列隔开。跨越重复片段的重组可以产生一个带有复制起点的质粒和/或一个带有功能性T抗原基因的质粒,该基因将驱动两者的复制。将这种构建体导入非洲绿猴肾细胞,不进行共感染,建立了一种可以明确解释重组或基因转换产物的条件。我们发现大多数重建反应是非保守的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/76d3/367806/db203ab4f4fa/molcellb00091-0244-a.jpg

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