关于单纯疱疹病毒1型单链DNA结合蛋白(ICP8)的链同化机制
On the mechanism of strand assimilation by the herpes simplex virus type-1 single-strand DNA-binding protein (ICP8).
作者信息
Nimonkar Amitabh V, Boehmer Paul E
机构信息
Department of Biochemistry and Molecular Biology, University of Miami School of Medicine, PO Box 016129, Miami, FL 33101-6129, USA.
出版信息
Nucleic Acids Res. 2003 Sep 15;31(18):5275-81. doi: 10.1093/nar/gkg740.
Abstract
ICP8, the herpes simplex virus type-1 encoded single-strand DNA (ssDNA)-binding protein, promotes the assimilation of a single-stranded DNA molecule into a homologous duplex plasmid resulting in the formation of a displacement loop. Here we examine the mechanism of this process. In contrast to the RecA-type recombinases that catalyze strand invasion via an active search for homology, ICP8 acts by a salt-dependent strand annealing mechanism. The active species in this reaction is a ssDNA:ICP8 nucleoprotein filament. There appears to be no requirement for ICP8 to interact with the acceptor DNA. At higher concentrations, ICP8 promotes the reverse reaction, presumably owing to its helix destabilizing activity. ICP8-mediated strand assimilation imparts single-stranded character onto the acceptor DNA, consistent with the formation of a displacement loop. These data suggest that the recombination activity of ICP8 is similar to the mechanism of eukaryotic Rad52.
摘要
ICP8是单纯疱疹病毒1型编码的单链DNA(ssDNA)结合蛋白,它促进单链DNA分子与同源双链质粒的同化作用,从而导致置换环的形成。在此我们研究这一过程的机制。与通过主动寻找同源性来催化链侵入的RecA型重组酶不同,ICP8通过一种依赖盐的链退火机制起作用。该反应中的活性物质是ssDNA:ICP8核蛋白丝。似乎不需要ICP8与受体DNA相互作用。在较高浓度下,ICP8促进逆向反应,大概是由于其螺旋去稳定化活性。ICP8介导的链同化作用使受体DNA具有单链特征,这与置换环的形成一致。这些数据表明ICP8的重组活性类似于真核生物Rad52的机制。
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