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2
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Nucleic Acids Res. 2019 Feb 20;47(3):1211-1224. doi: 10.1093/nar/gky1188.
3
A Transcriptomics Approach To Unveiling the Mechanisms of Evolution towards Fluconazole Resistance of a Clinical Isolate.一种转录组学方法揭示临床分离株向氟康唑耐药进化的机制。
Antimicrob Agents Chemother. 2018 Dec 21;63(1). doi: 10.1128/AAC.00995-18. Print 2019 Jan.
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Fungal Resistance to Echinocandins and the MDR Phenomenon in .真菌对棘白菌素的耐药性及多重耐药现象
J Fungi (Basel). 2018 Sep 1;4(3):105. doi: 10.3390/jof4030105.
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Unveiling the transcriptional control of pleiotropic drug resistance in Saccharomyces cerevisiae: Contributions of André Goffeau and his group.揭示酿酒酵母中多药耐药性的转录调控:安德烈·戈弗雷及其团队的贡献。
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Integrated analysis of the yeast NADPH-regulator Stb5 reveals distinct differences in NADPH requirements and regulation in different states of yeast metabolism.酵母 NADPH 调节剂 Stb5 的综合分析揭示了不同酵母代谢状态下 NADPH 需求和调节的明显差异。
FEMS Yeast Res. 2018 Dec 1;18(8). doi: 10.1093/femsyr/foy091.
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Multiple interfaces control activity of the Candida glabrata Pdr1 transcription factor mediating azole drug resistance.多个界面控制介导唑类药物耐药性的 Candida glabrata Pdr1 转录因子的活性。
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Transcriptional Profiling of Reveals the Impact of Variation of a Single Transcription Factor on Differential Gene Expression in 4NQO, Fermentable, and Nonfermentable Carbon Sources.[具体研究对象]的转录谱分析揭示了单个转录因子的变异对4NQO、可发酵碳源和不可发酵碳源中差异基因表达的影响。
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10
Different Toxicity Mechanisms for Citrinin and Ochratoxin A Revealed by Transcriptomic Analysis in Yeast.转录组分析揭示酵母中桔霉素和赭曲霉毒素A的不同毒性机制
Toxins (Basel). 2016 Sep 22;8(10):273. doi: 10.3390/toxins8100273.

活细胞检测揭示出出芽酵母中多药反应的选择性和敏感性。

Live-cell assays reveal selectivity and sensitivity of the multidrug response in budding yeast.

机构信息

Department of Biotechnology, Instituto de Biología Molecular y Celular de Plantas, Universitat Politècnica de València, 46022 Valencia, Spain.

Department of Molecular and Cellular Pathology and Therapy, Instituto de Biomedicina de Valencia IBV-CSIC, 46010 Valencia, Spain.

出版信息

J Biol Chem. 2019 Aug 30;294(35):12933-12946. doi: 10.1074/jbc.RA119.009291. Epub 2019 Jul 11.

DOI:10.1074/jbc.RA119.009291
PMID:31296662
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6721934/
Abstract

Pleiotropic drug resistance arises by the enhanced extrusion of bioactive molecules and is present in a wide range of organisms, ranging from fungi to human cells. A key feature of this adaptation is the sensitive detection of intracellular xenobiotics by transcriptional activators, activating expression of multiple drug exporters. Here, we investigated the selectivity and sensitivity of the budding yeast () multidrug response to better understand how differential drug recognition leads to specific activation of drug exporter genes and to drug resistance. Applying live-cell luciferase reporters, we demonstrate that the , , and transporter genes respond to different mycotoxins, menadione, and hydrogen peroxide in a distinguishable manner and with characteristic amplitudes, dynamics, and sensitivities. These responses correlated with differential sensitivities of the respective transporter mutants to the specific xenobiotics. We further establish a binary vector system, enabling quantitative determination of xenobiotic-transcription factor (TF) interactions in real time. Applying this system we found that the TFs Pdr1, Pdr3, Yrr1, Stb5, and Pdr8 have largely different drug recognition patterns. We noted that Pdr1 is the most promiscuous activator, whereas Yrr1 and Stb5 are selective for ochratoxin A and hydrogen peroxide, respectively. We also show that Pdr1 is rapidly degraded after xenobiotic exposure, which leads to a desensitization of the Pdr1-specific response upon repeated activation. The findings of our work indicate that in the yeast multidrug system, several transcriptional activators with distinguishable selectivities trigger differential activation of the transporter genes.

摘要

多药耐药性是通过增强生物活性分子的外排而产生的,存在于从真菌到人类细胞的广泛生物体中。这种适应的一个关键特征是转录激活因子对细胞内异源生物的敏感检测,激活多种药物外排泵的表达。在这里,我们研究了酿酒酵母()多药反应的选择性和敏感性,以更好地理解不同的药物识别如何导致药物外排基因的特异性激活和耐药性。通过应用活细胞荧光素酶报告基因,我们证明了 、 、 和 转运基因以可区分的方式和具有特征幅度、动力学和敏感性对不同的霉菌毒素、甲萘醌和过氧化氢作出反应。这些反应与各自转运突变体对特定外源性物质的差异敏感性相关。我们进一步建立了一个二元载体系统,能够实时定量测定外源性物质-转录因子(TF)相互作用。应用该系统,我们发现 TFs Pdr1、Pdr3、Yrr1、Stb5 和 Pdr8 具有截然不同的药物识别模式。我们注意到 Pdr1 是最混杂的激活剂,而 Yrr1 和 Stb5 分别对赭曲霉毒素 A 和过氧化氢具有选择性。我们还表明,Pdr1 在暴露于外源性物质后会迅速降解,这导致 Pdr1 特异性反应在重复激活时脱敏。我们工作的发现表明,在酵母多药系统中,几个具有可区分选择性的转录激活因子触发了转运基因的差异激活。