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药物诱导的离子动态平衡的功能基因组学鉴定了酵母中铁和锌调控子的新型调控串扰。

Functional genomics of drug-induced ion homeostasis identifies a novel regulatory crosstalk of iron and zinc regulons in yeast.

机构信息

Medical University Vienna, Max F. Perutz Laboratories, Campus Vienna Biocenter, A-1030 Vienna, Austria.

出版信息

OMICS. 2010 Dec;14(6):651-63. doi: 10.1089/omi.2010.0031. Epub 2010 Aug 9.

Abstract

Pyrrolidine dithiocarbamate (PDTC), a known inhibitor of NFκB activation, has antioxidative as well as antiviral activities. PDTC is effective against several virus families, indicating that its antiviral mechanism targets host rather than viral functions. To investigate its mode of action, we used baker's yeast as a simple eukaryotic model system and two types of genome-wide analysis. First, expression profiling using whole-genome DNA microarrays identifies more than 200 genes differentially regulated upon PDTC exposure. Interestingly, the Aft1-dependent iron regulon is a main target of PDTC, indicating a lack of iron availability. Moreover, the PDTC-caused zinc influx triggers a strong regulatory effect on zinc transporters due to the cytoplasmic zinc excess. Second, phenotypic screening the EUROSCARF collection for PDTC hypersensitivity identifies numerous mutants implicated in vacuolar maintenance, acidification as well as in transport, mitochondrial organization, and translation. Notably, the screening data indicate significant overlaps of PDTC-sensitive genes and those mediating zinc tolerance. Hence, we show that PDTC induces cytoplasmic zinc excess, eliciting vacuolar detoxification, which in turn, disturbs iron homeostasis and activates the iron-dependent regulator Aft1. Our work reveals a complex crosstalk in yeast ion homeostasis and the underlying regulatory networks.

摘要

吡咯烷二硫代氨基甲酸盐(PDTC)是一种已知的 NFκB 激活抑制剂,具有抗氧化和抗病毒活性。PDTC 对多种病毒家族有效,表明其抗病毒机制针对宿主而非病毒功能。为了研究其作用机制,我们使用面包酵母作为简单的真核模型系统,并进行了两种类型的全基因组分析。首先,使用全基因组 DNA 微阵列进行表达谱分析,确定了超过 200 个在 PDTC 暴露后差异调节的基因。有趣的是,Aft1 依赖性铁调节子是 PDTC 的主要靶标,表明铁的可用性不足。此外,PDTC 引起的锌内流由于细胞质锌过剩,对锌转运体产生强烈的调节作用。其次,对 EUROSCARF 集合进行 PDTC 敏感性表型筛选,鉴定出许多与液泡维持、酸化以及运输、线粒体组织和翻译有关的突变体。值得注意的是,筛选数据表明 PDTC 敏感基因与介导锌耐受的基因之间存在显著重叠。因此,我们表明 PDTC 诱导细胞质锌过剩,引发液泡解毒,从而扰乱铁稳态并激活铁依赖性调节剂 Aft1。我们的工作揭示了酵母离子稳态和潜在调节网络中的复杂串扰。

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