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大肠杆菌DNA聚合酶III全酶与引发型DNA在无ATP情况下形成的起始复合物的性质

Properties of initiation complexes formed between Escherichia coli DNA polymerase III holoenzyme and primed DNA in the absence of ATP.

作者信息

Kwon-Shin O, Bodner J B, McHenry C S, Bambara R A

出版信息

J Biol Chem. 1987 Feb 15;262(5):2121-30.

PMID:3546285
Abstract

In the presence of ATP, the beta subunit of the Escherichia coli DNA polymerase III holoenzyme can induce a stable initiation complex with the other holoenzyme subunits and primed DNA that is capable of highly processive synthesis. We have recently demonstrated that the ATP requirement for processive synthesis can be bypassed by an excess of the beta subunit (Crute, J., LaDuca, R., Johanson, K., McHenry, C., and Bambara, R. (1983) J. Biol. Chem. 258, 11344-11349). To examine the complex formed with excess beta subunit, and the lengths of the products of processive synthesis, we have designed a uniquely primed DNA template. Poly(dA)4000 was tailed with dCTP by terminal deoxynucleotidyl transferase and the resulting template annealed to oligo(dG)12-18. In the presence of excess beta, the lengths of processively extended primers nearly equaled the full-length of the DNA template. Similar length synthesis occurred in the presence or absence of spermidine or single-stranded DNA-binding protein. When the beta subunit was present at normal holoenzyme stoichiometry it could induce highly processive synthesis without ATP, although inefficiently. Both ATP and excess beta increased the amount of initiation complex formation, but complexes produced with excess beta did so without the time delay observed with ATP, suggesting different mechanisms for formation. Almost 50% of initiation complexes formed without ATP survived a 30-min incubation with anti-beta IgG, reflecting a stability similar to those formed with ATP. The ability to form initiation complexes in the absence of ATP permitted the demonstration that cycling of the holoenzyme to a new primer, after chain termination with a dideoxynucleotide, is not affected by the presence of ATP.

摘要

在有ATP存在的情况下,大肠杆菌DNA聚合酶III全酶的β亚基可与其他全酶亚基及引发的DNA形成稳定的起始复合物,该复合物能够进行高度连续的合成。我们最近证明,过量的β亚基可绕过连续合成对ATP的需求(克鲁特,J.,拉杜卡,R.,约翰森,K.,麦克亨利,C.,和班巴拉,R.(1983年)《生物化学杂志》258卷,11344 - 11349页)。为了研究与过量β亚基形成的复合物以及连续合成产物的长度,我们设计了一种独特的引发DNA模板。用末端脱氧核苷酸转移酶给聚(dA)4000接上dCTP尾巴,然后将所得模板与寡聚(dG)12 - 18退火。在过量β亚基存在的情况下,连续延伸引物的长度几乎与DNA模板的全长相等。在有或没有亚精胺或单链DNA结合蛋白存在的情况下,都发生了类似长度的合成。当β亚基以正常全酶化学计量存在时,它可在没有ATP的情况下诱导高度连续的合成,尽管效率不高。ATP和过量的β亚基都增加了起始复合物形成的量,但过量β亚基产生的复合物形成时没有观察到ATP存在时的时间延迟,这表明形成机制不同。在没有ATP的情况下形成的起始复合物中,近50%在用抗β免疫球蛋白孵育30分钟后仍存活,这反映出其稳定性与有ATP时形成的复合物相似。在没有ATP的情况下形成起始复合物的能力使得能够证明,在用双脱氧核苷酸终止链后,全酶循环到新引物的过程不受ATP存在的影响。

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