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本文引用的文献

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An evolutionary biochemist's perspective on promiscuity.一位进化生物化学家对滥交的看法。
Trends Biochem Sci. 2015 Feb;40(2):72-8. doi: 10.1016/j.tibs.2014.12.004. Epub 2015 Jan 5.
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TcaR-ssDNA complex crystal structure reveals new DNA binding mechanism of the MarR family proteins.TcaR-ssDNA 复合物晶体结构揭示了 MarR 家族蛋白的新 DNA 结合机制。
Nucleic Acids Res. 2014 Apr;42(8):5314-21. doi: 10.1093/nar/gku128. Epub 2014 Feb 14.
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The oxidation-sensing regulator (MosR) is a new redox-dependent transcription factor in Mycobacterium tuberculosis.氧化感应调节蛋白(MosR)是结核分枝杆菌中一种新的依赖于氧化还原的转录因子。
J Biol Chem. 2012 Nov 2;287(45):37703-12. doi: 10.1074/jbc.M112.388611. Epub 2012 Sep 18.
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Characterization of transport proteins for aromatic compounds derived from lignin: benzoate derivative binding proteins.木质素衍生芳香族化合物转运蛋白的特性: 苯甲酸衍生物结合蛋白。
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Anaerobic p-coumarate degradation by Rhodopseudomonas palustris and identification of CouR, a MarR repressor protein that binds p-coumaroyl coenzyme A.沼泽红假单胞菌对厌氧型对香豆酸的降解作用及 CouR 的鉴定,CouR 是一种 MarR 型阻遏蛋白,可与对香豆酰辅酶 A 结合。
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Crystal structure of the zinc-dependent MarR family transcriptional regulator AdcR in the Zn(II)-bound state.锌依赖型 MarR 家族转录调控因子 AdcR 在 Zn(II)结合态下的晶体结构。
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High-throughput protein purification and quality assessment for crystallization.高通量蛋白质纯化及其用于结晶的质量评估。
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Crystal structures of SlyA protein, a master virulence regulator of Salmonella, in free and DNA-bound states.SlyA 蛋白的晶体结构,一种沙门氏菌的主要毒力调节因子,分别处于自由态和与 DNA 结合态。
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MarR homologs with urate-binding signature.具有尿酸结合特征的 MarR 同源物。
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The structure of the CRISPR-associated protein Csa3 provides insight into the regulation of the CRISPR/Cas system.CRISPR 相关蛋白 Csa3 的结构为研究 CRISPR/Cas 系统的调控机制提供了线索。
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芳香族化合物如何阻断HcaR分解代谢调节因子与DNA的结合。

How Aromatic Compounds Block DNA Binding of HcaR Catabolite Regulator.

作者信息

Kim Youngchang, Joachimiak Grazyna, Bigelow Lance, Babnigg Gyorgy, Joachimiak Andrzej

机构信息

From the Midwest Center for Structural Genomics and Structural Biology Center, Biosciences, Argonne National Laboratory, Argonne, Illinois 60439.

From the Midwest Center for Structural Genomics and.

出版信息

J Biol Chem. 2016 Jun 17;291(25):13243-56. doi: 10.1074/jbc.M115.712067. Epub 2016 Apr 25.

DOI:10.1074/jbc.M115.712067
PMID:27129205
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4933237/
Abstract

Bacterial catabolism of aromatic compounds from various sources including phenylpropanoids and flavonoids that are abundant in soil plays an important role in the recycling of carbon in the ecosystem. We have determined the crystal structures of apo-HcaR from Acinetobacter sp. ADP1, a MarR/SlyA transcription factor, in complexes with hydroxycinnamates and a specific DNA operator. The protein regulates the expression of the hca catabolic operon in Acinetobacter and related bacterial strains, allowing utilization of hydroxycinnamates as sole sources of carbon. HcaR binds multiple ligands, and as a result the transcription of genes encoding several catabolic enzymes is increased. The 1.9-2.4 Å resolution structures presented here explain how HcaR recognizes four ligands (ferulate, 3,4-dihydroxybenzoate, p-coumarate, and vanillin) using the same binding site. The ligand promiscuity appears to be an adaptation to match a broad specificity of hydroxycinnamate catabolic enzymes while responding to toxic thioester intermediates. Structures of apo-HcaR and in complex with a specific DNA hca operator when combined with binding studies of hydroxycinnamates show how aromatic ligands render HcaR unproductive in recognizing a specific DNA target. The current study contributes to a better understanding of the hca catabolic operon regulation mechanism by the transcription factor HcaR.

摘要

包括土壤中丰富的苯丙烷类化合物和黄酮类化合物在内的各种来源的芳香族化合物的细菌分解代谢,在生态系统的碳循环中起着重要作用。我们已经确定了来自不动杆菌属ADP1的脱辅基HcaR的晶体结构,它是一种MarR/SlyA转录因子,与羟基肉桂酸酯和特定的DNA操纵子形成复合物。该蛋白调节不动杆菌和相关细菌菌株中hca分解代谢操纵子的表达,使羟基肉桂酸酯能够作为唯一的碳源被利用。HcaR结合多种配体,结果增加了几种分解代谢酶编码基因的转录。这里给出的分辨率为1.9 - 2.4 Å的结构解释了HcaR如何利用相同的结合位点识别四种配体(阿魏酸、3,4 - 二羟基苯甲酸、对香豆酸和香草醛)。配体的混杂性似乎是一种适应性变化,以匹配羟基肉桂酸酯分解代谢酶的广泛特异性,同时应对有毒的硫酯中间体。脱辅基HcaR以及与特定DNA hca操纵子形成复合物的结构,与羟基肉桂酸酯的结合研究相结合,表明芳香族配体如何使HcaR无法有效识别特定的DNA靶点。当前的研究有助于更好地理解转录因子HcaR对hca分解代谢操纵子的调控机制。