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嗜热真细菌海栖热袍菌(Thermotoga maritima)的DnaA同源物以ATP依赖的方式与一个最小的149碱基对的起始区域形成开放复合物。

The DnaA homolog of the hyperthermophilic eubacterium Thermotoga maritima forms an open complex with a minimal 149-bp origin region in an ATP-dependent manner.

作者信息

Ozaki Shogo, Fujimitsu Kazuyuki, Kurumizaka Hitoshi, Katayama Tsutomu

机构信息

Department of Molecular Biology, Graduate School of Pharmaceutical Sciences, Kyushu University, 3-1-1 Maidashi, Higashi-ku, Fukuoka 812-8582, Japan.

出版信息

Genes Cells. 2006 Apr;11(4):425-38. doi: 10.1111/j.1365-2443.2006.00950.x.

Abstract

In Escherichia coli, ATP-DnaA, but not ADP-DnaA, forms an initiation complex that undergoes site-specific duplex DNA unwinding, open complex formation. However, it remains unclear how highly the ATP-dependent activation of the initiation factor is conserved in evolution. The hyperthermophile Thermotoga maritima is one of the most ancient eubacteria in evolution. Here, we show that the DnaA homolog (tmaDnaA) of this bacterium forms open complexes with the predicted origin region (tma-oriC) in vitro. TmaDnaA has a strong and specific affinity for ATP/ADP as well as for 12-mer repeating sequences within the tma-oriC. Unlike ADP-tmaDnaA, ATP-tmaDnaA is highly cooperative in DNA binding and forms open complexes in a manner that depends on temperature and the superhelical tension of the tma-oriC-bearing plasmid. The minimal tma-oriC required for unwinding is a 149-bp region containing five repeats of the 12-mer sequence and two AT-rich 9-mer repeats. TmaDnaA-binding to the 12-mer motif provokes DNA bending. The 9-mer region is the duplex-unwinding site. The tmaDnaA-binding and unwinding motifs of tma-oriC share sequence homology with corresponding archaeal and eukaryotic sequences. These findings suggest that the ATP-dependent molecular switch of the initiator and the mechanisms in the replication initiation complex are highly conserved in eubacterial evolution.

摘要

在大肠杆菌中,ATP-DnaA而非ADP-DnaA形成起始复合物,该复合物会经历位点特异性双链DNA解旋及开放复合物的形成。然而,起始因子的ATP依赖性激活在进化过程中的保守程度仍不清楚。嗜热栖热菌是进化过程中最古老的真细菌之一。在此,我们表明该细菌的DnaA同源物(tmaDnaA)在体外与预测的起始区域(tma-oriC)形成开放复合物。TmaDnaA对ATP/ADP以及tma-oriC内的12聚体重复序列具有强烈且特异性的亲和力。与ADP-tmaDnaA不同,ATP-tmaDnaA在DNA结合方面具有高度协同性,并以依赖于温度和携带tma-oriC的质粒的超螺旋张力的方式形成开放复合物。解旋所需的最小tma-oriC是一个149 bp的区域,包含12聚体序列的五个重复以及两个富含AT的9聚体重复。TmaDnaA与12聚体基序的结合会引发DNA弯曲。9聚体区域是双链解旋位点。tma-oriC的tmaDnaA结合和解旋基序与相应的古细菌和真核生物序列具有序列同源性。这些发现表明起始因子的ATP依赖性分子开关以及复制起始复合物中的机制在真细菌进化中高度保守。

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