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剖析细菌和古细菌中DNA结合转录因子的蛋白质结构

Dissecting the protein architecture of DNA-binding transcription factors in bacteria and archaea.

作者信息

Rivera-Gómez Nancy, Martínez-Núñez Mario Alberto, Pastor Nina, Rodriguez-Vazquez Katya, Perez-Rueda Ernesto

机构信息

Centro de Investigaciones en Biotecnología, Universidad Autónoma del Estado de Morelos, Cuernavaca, México.

Laboratorio de Estudios Ecogenómicos, Facultad de Ciencias, Unidad Académica de Ciencias y Tecnología de Yucatán, Universidad Nacional Autónoma de México, Mérida, Yucatán, México.

出版信息

Microbiology (Reading). 2017 Aug;163(8):1167-1178. doi: 10.1099/mic.0.000504. Epub 2017 Aug 17.

DOI:10.1099/mic.0.000504
PMID:28777072
Abstract

Gene regulation at the transcriptional level is a central process in all organisms where DNA-binding transcription factors play a fundamental role. This class of proteins binds specifically at DNA sequences, activating or repressing gene expression as a function of the cell's metabolic status, operator context and ligand-binding status, among other factors, through the DNA-binding domain (DBD). In addition, TFs may contain partner domains (PaDos), which are involved in ligand binding and protein-protein interactions. In this work, we systematically evaluated the distribution, abundance and domain organization of DNA-binding TFs in 799 non-redundant bacterial and archaeal genomes. We found that the distributions of the DBDs and their corresponding PaDos correlated with the size of the genome. We also identified specific combinations between the DBDs and their corresponding PaDos. Within each class of DBDs there are differences in the actual angle formed at the dimerization interface, responding to the presence/absence of ligands and/or crystallization conditions, setting the orientation of the resulting helices and wings facing the DNA. Our results highlight the importance of PaDos as central elements that enhance the diversity of regulatory functions in all bacterial and archaeal organisms, and our results also demonstrate the role of PaDos in sensing diverse signal compounds. The highly specific interactions between DBDs and PaDos observed in this work, together with our structural analysis highlighting the difficulty in predicting both inter-domain geometry and quaternary structure, suggest that these systems appeared once and evolved with diverse duplication events in all the analysed organisms.

摘要

转录水平的基因调控是所有生物体中的核心过程,其中DNA结合转录因子发挥着基本作用。这类蛋白质特异性结合DNA序列,根据细胞的代谢状态、操纵子环境和配体结合状态等因素,通过DNA结合结构域(DBD)激活或抑制基因表达。此外,转录因子可能包含参与配体结合和蛋白质-蛋白质相互作用的伙伴结构域(PaDos)。在这项工作中,我们系统地评估了799个非冗余细菌和古菌基因组中DNA结合转录因子的分布、丰度和结构域组织。我们发现DBD及其相应的PaDos的分布与基因组大小相关。我们还确定了DBD及其相应的PaDos之间的特定组合。在每一类DBD中,二聚化界面处形成的实际角度存在差异,这取决于配体的存在与否和/或结晶条件,决定了所得螺旋和侧翼面对DNA的方向。我们的结果突出了PaDos作为增强所有细菌和古菌生物体调控功能多样性的核心元件的重要性,并且我们的结果还证明了PaDos在感知多种信号化合物中的作用。在这项工作中观察到的DBD和PaDos之间高度特异性相互作用,以及我们强调预测结构域间几何形状和四级结构都存在困难的结构分析,表明这些系统在所有分析的生物体中一旦出现就随着不同的复制事件而进化。

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