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The adenovirus DNA binding protein enhances intermolecular DNA renaturation but inhibits intramolecular DNA renaturation.

机译:腺病毒DNA结合蛋白可增强分子间DNA复性,但可抑制分子内DNA复性。

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摘要

The Adenovirus DNA binding protein (DBP) imposes a regular, rigid and extended conformation on single stranded DNA (ssDNA) and removes secondary structure. Here we show that DBP promotes renaturation of complementary single DNA strands. Enhancement of intermolecular renaturation is sequence independent, can be observed over a broad range of ionic conditions and occurs only when the DNA strands are completely covered with DBP. When one strand of DNA is covered with DBP and its complementary strand with T4 gene 32 protein, renaturation is still enhanced compared to protein-free DNA, indicating that the structures of both protein-DNA complexes are compatible for renaturation. In contrast to promoting intermolecular renaturation, DBP strongly inhibits intramolecular renaturation required for the formation of a panhandle from an ssDNA molecule with an inverted terminal repeat. We explain this by the rigidity of an ssDNA-DBP complex. These results will be discussed in view of the crystal structure of DBP that has recently been determined.
机译:腺病毒DNA结合蛋白(DBP)对单链DNA(ssDNA)施加规则的,刚性的和延伸的构象,并去除二级结构。在这里,我们表明DBP可以促进互补的单个DNA链的复性。分子间复性的增强与序列无关,可以在广泛的离子条件下观察到,并且仅当DNA链完全被DBP覆盖时才会发生。当一条DNA链被DBP覆盖,其互补链被T4基因32蛋白覆盖时,与无蛋白质的DNA相比,复性仍然增强,这表明两种蛋白质-DNA复合物的结构都适合复性。与促进分子间复性相反,DBP强烈抑制由具有反向末端重复的ssDNA分子形成泛柄所需的分子内复性。我们通过ssDNA-DBP复合体的刚性来解释这一点。鉴于最近确定的DBP晶体结构,将讨论这些结果。

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