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生物素阻遏物 - 生物素操纵基因复合物组装过程中位点特异性DNA结合与蛋白质二聚化的偶联。

Coupling of site-specific DNA binding to protein dimerization in assembly of the biotin repressor-biotin operator complex.

作者信息

Streaker E D, Beckett D

机构信息

Department of Chemistry and Biochemistry, University of Maryland Baltimore County, 1000 Hilltop Circle, Baltimore, Maryland 21250, USA.

出版信息

Biochemistry. 1998 Mar 3;37(9):3210-9. doi: 10.1021/bi9715019.

Abstract

The Escherichia coli repressor of biotin biosynthesis, BirA, binds site-specifically to the biotin operator, a 40 base pair imperfect inverted palindrome. Two repressor monomers have been shown to bind to the two operator half-sites. Analysis of results of quantitative DNase I footprint titrations performed on the wild-type biotin operator template indicate that binding is well described by a cooperative mechanism. The data obtained from these studies were, however, insufficient to independently resolve all of the energetic parameters associated with cooperative binding of the two repressor monomers to the operator site. In this work, to further dissect the energetics of assembly of the biotin repressor-biotin operator complex, measurements of binding of BirA to four bioO variants designed to reduce the valency of repressor binding from 2 to 1 have been performed. Results of these measurements indicate, as was found with the wild-type biotin operator template, that two repressor monomers bind simultaneously to the two half-sites of all variant operators. Protein dimerization and DNA binding are thus obligatorily coupled in the biotin repressor system. Furthermore, the results suggest that, in the context of a cooperative binding mechanism, the cooperative free energy associated with the biotin repressor-biotin operator interaction is significantly more favorable than the previously estimated -2 kcal/mol.

摘要

生物素生物合成的大肠杆菌阻遏物BirA能位点特异性地结合生物素操纵基因,它是一个40个碱基对的不完全反向回文序列。已有研究表明,两个阻遏物单体可结合到操纵基因的两个半位点上。对野生型生物素操纵基因模板进行的定量DNase I足迹滴定结果分析表明,结合作用可用协同机制很好地描述。然而,从这些研究中获得的数据不足以独立解析与两个阻遏物单体协同结合到操纵基因位点相关的所有能量参数。在这项工作中,为了进一步剖析生物素阻遏物 - 生物素操纵基因复合物组装的能量学,已对四个旨在将阻遏物结合价从2降低到1的bioO变体进行了BirA结合测量。这些测量结果表明,与野生型生物素操纵基因模板的情况一样,两个阻遏物单体同时结合到所有变体操纵基因的两个半位点上。因此,在生物素阻遏物系统中,蛋白质二聚化和DNA结合必然是耦合的。此外,结果表明,在协同结合机制的背景下,与生物素阻遏物 - 生物素操纵基因相互作用相关的协同自由能比先前估计的-2千卡/摩尔更有利。

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