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Strand invasion promoted by recombination protein beta of coliphage lambda.

机译:噬菌体λ的重组蛋白β促进了链侵袭。

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Studies of phage lambda in vivo have indicated that its own recombination enzymes, beta protein and lambda exonuclease, are capable of catalyzing two dissimilar pathways of homologous recombination that are widely distributed in nature: single-strand annealing and strand invasion. The former is an enzymatic splicing of overlapping ends of broken homologous DNA molecules, whereas the latter is characterized by the formation of a three-stranded synaptic intermediate and subsequent strand exchange. Previous studies in vitro have shown that beta protein has annealing activity, and that lambda exonuclease, acting on branched substrates, can produce a perfect splice that requires only ligation for completion. The present study shows that beta protein can initiate strand invasion in vitro, as evidenced both by the formation of displacement loops (D-loops) in superhelical DNA and by strand exchange between colinear single-stranded and double-stranded molecules. Thus, beta protein can catalyze steps that are central to both strand annealing and strand invasion pathways of recombination. These observations add beta protein to a set of diverse proteins that appear to promote recognition of homology by a unitary mechanism governed by the intrinsic dynamic properties of base pairs in DNA.
机译:体内噬菌体λ的研究表明,其自身的重组酶β蛋白和λ核酸外切酶能够催化自然界中广泛分布的两种不同的同源重组途径:单链退火和链入侵。前者是断裂的同源DNA分子重叠末端的酶切拼接,而后者的特征是形成三链突触中间物并随后进行链交换。以前的体外研究表明,β蛋白具有退火活性,作用在分支底物上的λ核酸外切酶可以产生仅需连接即可完成的完美剪接。本研究表明,β蛋白可以在体外引发链条入侵,既可以通过超螺旋DNA中置换环(D-loop)的形成,又可以通过共线单链和双链分子之间的链交换来证明。因此,β蛋白可以催化链退火和链入侵重组途径都至关重要的步骤。这些发现将β蛋白添加到一组多样化的蛋白中,这些蛋白似乎通过统一机制来促进同源性的识别,该统一机制受DNA中碱基对的内在动态特性支配。

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