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大肠杆菌中转座靶点的微阵列分析:转录的影响

Microarray analysis of transposition targets in Escherichia coli: the impact of transcription.

作者信息

Manna Dipankar, Breier Adam M, Higgins N Patrick

机构信息

Department of Biochemistry and Molecular Genetics, University of Alabama at Birmingham, Birmingham, AL 35294, USA.

出版信息

Proc Natl Acad Sci U S A. 2004 Jun 29;101(26):9780-5. doi: 10.1073/pnas.0400745101. Epub 2004 Jun 21.

Abstract

Transposable elements have influenced the genetic and physical composition of all modern organisms. Defining how different transposons select target sites is critical for understanding the biochemical mechanism of this type of recombination and the impact of mobile genes on chromosome structure and function. Phage Mu replicates in Gram-negative bacteria using an extremely efficient transposition reaction. Replicated copies are excised from the chromosome and packaged into virus particles. Each viral genome plus several hundred base pairs of host DNA covalently attached to the prophage right end is packed into a virion. To study Mu transposition preferences, we used DNA microarray technology to measure the abundance of >4,000 Escherichia coli genes in purified Mu phage DNA. Insertion hot- and cold-spot genes were found throughout the genome, reflecting >1,000-fold variation in utilization frequency. A moderate preference was observed for genes near the origin compared to terminus of replication. Large biases were found at hot and cold spots, which often include several consecutive genes. Efficient transcription of genes had a strong negative influence on transposition. Our results indicate that local chromosome structure is more important than DNA sequence in determining Mu target-site selection.

摘要

转座元件影响了所有现代生物的遗传和物理组成。明确不同转座子如何选择靶位点对于理解这类重组的生化机制以及移动基因对染色体结构和功能的影响至关重要。噬菌体Mu利用一种极其高效的转座反应在革兰氏阴性细菌中进行复制。复制后的拷贝从染色体上切除并包装进病毒颗粒。每个病毒基因组加上共价连接到原噬菌体右端的几百个碱基对的宿主DNA被包装进一个病毒粒子。为了研究Mu的转座偏好,我们使用DNA微阵列技术来测量纯化的Mu噬菌体DNA中4000多个大肠杆菌基因的丰度。在整个基因组中发现了插入热点和冷点基因,这反映了利用频率超过1000倍的差异。与复制终点相比,观察到对复制起点附近基因有一定偏好。在热点和冷点发现了很大的偏差,这些热点和冷点通常包括几个连续的基因。基因的高效转录对转座有强烈的负面影响。我们的结果表明,在决定Mu靶位点选择时,局部染色体结构比DNA序列更重要。

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