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扩展规则:一种更新的共识操作子位点,用于细菌铜输出系统阻遏物的 CopR-CopY 家族。

Rules of Expansion: an Updated Consensus Operator Site for the CopR-CopY Family of Bacterial Copper Exporter System Repressors.

机构信息

Department of Immunobiology, University of Arizona, Tucson, Arizona, USA.

BIO5 Institute, University of Arizona, Tucson, Arizona, USA.

出版信息

mSphere. 2020 May 27;5(3):e00411-20. doi: 10.1128/mSphere.00411-20.

Abstract

Copper is broadly toxic to bacteria. As such, bacteria have evolved specialized copper export systems ( operons) often consisting of a DNA-binding/copper-responsive regulator (which can be a repressor or activator), a copper chaperone, and a copper exporter. For those bacteria using DNA-binding copper repressors, few studies have examined the regulation of this operon regarding the operator DNA sequence needed for repressor binding. In (the pneumococcus), CopY is the copper repressor for the operon. Previously, homologs of pneumococcal CopY have been characterized to bind a 10-base consensus sequence T/GACANNTGTA known as the box. Using this motif, we sought to determine whether genes outside the operon are also regulated by the CopY repressor, which was previously shown in We found that CopY did not bind to operators upstream of these candidate genes During this process, we found that the box sequence is necessary but not sufficient for CopY binding. Here, we propose an updated operator sequence for the operon to be ATTGACAAATGTAGAT binding CopY with a dissociation constant ( ) of ∼28 nM. We demonstrate strong cross-species interaction between some CopY proteins and CopY operators, suggesting strong evolutionary conservation. Taken together with our binding studies and bioinformatics data, we propose the consensus operator RNYKACANNYGTMRNY for the bacterial CopR-CopY copper repressor homologs. Many Gram-positive bacteria respond to copper stress by upregulating a copper export system controlled by a copper-sensitive repressor, CopR-CopY. The previous operator sequence for this family of proteins had been identified as TACANNTGTA. Here, using several recombinant proteins and mutations in various DNA fragments, we define those 10 bases as necessary but not sufficient for binding and in doing so, refine the operon operator to the 16-base sequence RNYKACANNTGTMRNY. Due to the sheer number of repressors that have been said to bind to the original 10 bases, including many antibiotic resistance repressors such as BlaI and MecI, we feel that this study highlights the need to reexamine many of these sites of the past and use added stringency for verifying operators in the future.

摘要

铜对细菌有广泛的毒性。因此,细菌已经进化出专门的铜输出系统(操纵子),通常由 DNA 结合/铜响应调节剂(可以是阻遏物或激活物)、铜伴侣和铜输出器组成。对于那些使用 DNA 结合铜阻遏物的细菌,很少有研究检查关于阻遏物结合所需的操纵子 DNA 序列的这种操纵子的调节。在肺炎球菌中,CopY 是 操纵子的铜阻遏物。以前,肺炎球菌 CopY 的同源物已被表征为结合称为 盒的 10 个碱基的共识序列 T/GACANNTGTA。使用此基序,我们试图确定 操纵子之外的基因是否也受到 CopY 阻遏物的调节,此前在 中已经显示。我们发现, CopY 不会与这些候选基因上游的 操纵子结合。在这个过程中,我们发现 盒序列对于 CopY 结合是必要的但不是充分的。在这里,我们提出了一个更新的 操纵子序列 ATTGACAAATGTAGAT,用于与 CopY 结合,解离常数( )为∼28 nM。我们证明了一些 CopY 蛋白和 CopY 操纵子之间的强交叉物种相互作用,表明了强烈的进化保守性。结合我们的结合研究和生物信息学数据,我们提出了细菌 CopR-CopY 铜阻遏物同源物的共识操纵子 RNYKACANNYGTMRNY。许多革兰氏阳性细菌通过上调由铜敏感阻遏物 CopR-CopY 控制的铜输出系统来应对铜应激。该蛋白家族的先前操纵子序列已被鉴定为 TACANNTGTA。在这里,我们使用几种重组蛋白和各种 DNA 片段中的突变,将这 10 个碱基定义为结合所必需的,但不是充分的,并在此过程中,将 操纵子的操纵子细化为 16 个碱基序列 RNYKACANNTGTMRNY。由于据称许多抗生素抗性阻遏物(如 BlaI 和 MecI)都结合了原始的 10 个碱基,因此,我们认为这项研究强调了需要重新检查过去的许多这些位点,并在将来为验证操作员增加严格性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5922/7253601/976d50f036e5/mSphere.00411-20-f0001.jpg

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