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质粒编码的转录阻遏物CopG未结合配体及结合其操纵基因时的结构。

The structure of plasmid-encoded transcriptional repressor CopG unliganded and bound to its operator.

作者信息

Gomis-Rüth F X, Solá M, Acebo P, Párraga A, Guasch A, Eritja R, González A, Espinosa M, del Solar G, Coll M

机构信息

Institut de Biologia Molecular de Barcelona, CSIC, Jordi Girona, 18-26, 08034 Barcelona, Spain.

出版信息

EMBO J. 1998 Dec 15;17(24):7404-15. doi: 10.1093/emboj/17.24.7404.

Abstract

The structure of the 45 amino acid transcriptional repressor, CopG, has been solved unliganded and bound to its target operator DNA. The protein, encoded by the promiscuous streptococcal plasmid pMV158, is involved in the control of plasmid copy number. The structure of this protein repressor, which is the shortest reported to date and the first isolated from a plasmid, has a homodimeric ribbon-helix-helix arrangement. It is the prototype for a family of homologous plasmid repressors. CopG cooperatively associates, completely protecting several turns on one face of the double helix in both directions from a 13-bp pseudosymmetric primary DNA recognition element. In the complex structure, one protein tetramer binds at one face of a 19-bp oligonucleotide, containing the pseudosymmetric element, with two beta-ribbons inserted into the major groove. The DNA is bent 60 degrees by compression of both major and minor grooves. The protein dimer displays topological similarity to Arc and MetJ repressors. Nevertheless, the functional tetramer has a unique structure with the two vicinal recognition ribbon elements at a short distance, thus inducing strong DNA bend. Further structural resemblance is found with helix-turn-helix regions of unrelated DNA-binding proteins. In contrast to these, however, the bihelical region of CopG has a role in oligomerization instead of DNA recognition. This observation unveils an evolutionary link between ribbon-helix-helix and helix-turn-helix proteins.

摘要

45个氨基酸的转录抑制因子CopG的结构已在未结合配体以及结合其靶标操纵子DNA的情况下得到解析。该蛋白由具有广泛宿主范围的链球菌质粒pMV158编码,参与质粒拷贝数的控制。这种蛋白抑制因子是迄今为止报道的最短的,也是首个从质粒中分离出来的,具有同二聚体的带状-螺旋-螺旋结构排列。它是同源质粒抑制因子家族的原型。CopG协同结合,从一个13碱基对的假对称一级DNA识别元件在双螺旋的一个面上双向完全保护几个螺旋。在复合物结构中,一个蛋白四聚体结合在一个含有假对称元件的19碱基对寡核苷酸的一个面上,有两条β-链插入到主沟中。DNA通过主沟和小沟的压缩弯曲60度。该蛋白二聚体与Arc和MetJ抑制因子在拓扑结构上相似。然而,功能性四聚体具有独特的结构,两个相邻的识别带状元件距离很短,从而导致强烈的DNA弯曲。在不相关的DNA结合蛋白的螺旋-转角-螺旋区域也发现了进一步的结构相似性。然而,与这些不同的是,CopG的双螺旋区域在寡聚化而非DNA识别中起作用。这一观察揭示了带状-螺旋-螺旋蛋白和螺旋-转角-螺旋蛋白之间的进化联系。

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