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噬菌体λ-td内含子模型系统中双链断裂介导的重组的同源性要求

Homology requirements for double-strand break-mediated recombination in a phage lambda-td intron model system.

作者信息

Parker M M, Court D A, Preiter K, Belfort M

机构信息

Molecular Genetics Program, Wadsworth Center, New York State Department of Health, Albany, New York 12201-2002, USA.

出版信息

Genetics. 1996 Jul;143(3):1057-68. doi: 10.1093/genetics/143.3.1057.

Abstract

Many group I introns encode endonucleases that promote intron homing by initiating a double-strand break-mediated homologous recombination event. A td intron-phage lambda model system was developed to analyze exon homology effects on intron homing and determine the role of the lambda 5'-3' exonuclease complex (Red alpha beta) in the repair event. Efficient intron homing depended on exon lengths in the 35- to 50-bp range, although homing levels remained significantly elevated above nonbreak-mediated recombination with as little as 10 bp of flanking homology. Although precise intron insertion was demonstrated with extremely limiting exon homology, the complete absence of one exon produced illegitimate events on the side of heterology. Interestingly, intron inheritance was unaffected by the presence of extensive heterology at the double-strand break in wild-type lambda, provided that sufficient homology between donor and recipient was present distal to the heterologous sequences. However, these events involving heterologous ends were absolutely dependent on an intact Red exonuclease system. Together these results indicate that heterologous sequences can participate in double-strand break-mediated repair and imply that intron transposition to heteroallelic sites might occur at break sites within regions of limited or no homology.

摘要

许多I类内含子编码内切核酸酶,这些内切核酸酶通过引发双链断裂介导的同源重组事件来促进内含子归巢。构建了一个td内含子-λ噬菌体模型系统,以分析外显子同源性对内含子归巢的影响,并确定λ 5'-3'外切核酸酶复合物(Red αβ)在修复事件中的作用。高效的内含子归巢取决于35至50个碱基对范围内的外显子长度,尽管侧翼同源性低至10个碱基对时,归巢水平仍显著高于非断裂介导的重组。虽然在极端有限的外显子同源性情况下也证明了精确的内含子插入,但一个外显子完全缺失会在异源侧产生异常事件。有趣的是,在野生型λ中,双链断裂处存在广泛的异源序列并不影响内含子遗传,前提是在异源序列远端供体和受体之间存在足够的同源性。然而,这些涉及异源末端的事件绝对依赖于完整的Red外切核酸酶系统。这些结果共同表明,异源序列可以参与双链断裂介导的修复,并暗示内含子可能会转座到有限同源或无同源区域内的断裂位点处的异等位基因位点。

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本文引用的文献

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Mechanisms of intron mobility.内含子移动的机制。
J Biol Chem. 1995 Dec 22;270(51):30237-40. doi: 10.1074/jbc.270.51.30237.
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Introns as mobile genetic elements.作为可移动遗传元件的内含子。
Annu Rev Biochem. 1993;62:587-622. doi: 10.1146/annurev.bi.62.070193.003103.
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