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调控因子控制酿酒酵母 IXR1 的转录由氧气水平:从需氧到缺氧的转录适应模型涉及 ROX1 和 IXR1 的交叉调控。

Regulatory factors controlling transcription of Saccharomyces cerevisiae IXR1 by oxygen levels: a model of transcriptional adaptation from aerobiosis to hypoxia implicating ROX1 and IXR1 cross-regulation.

机构信息

Departamento de Biología Celular y Molecular, Facultad de Ciencias, Universidad de A Coruña, 15071, Spain.

出版信息

Biochem J. 2009 Dec 14;425(1):235-43. doi: 10.1042/BJ20091500.

Abstract

Ixr1p from Saccharomyces cerevisiae has been previously studied because it binds to DNA containing intrastrand cross-links formed by the anticancer drug cisplatin. Ixr1p is also a transcriptional regulator of anaerobic/hypoxic genes, such as SRP1/TIR1, which encodes a stress-response cell wall manoprotein, and COX5B, which encodes the Vb subunit of the mitochondrial complex cytochrome c oxidase. However, factors controlling IXR1 expression remained unexplored. In the present study we show that IXR1 mRNA levels are controlled by oxygen availability and increase during hypoxia. In aerobiosis, low levels of IXR1 expression are maintained by Rox1p repression through the general co-repressor complex Tup1-Ssn6. Ixr1p itself is necessary for full IXR1 expression under hypoxic conditions. Deletion analyses have identified the region in the IXR1 promoter responsible for this positive auto-control (nucleotides -557 to -376). EMSA (electrophoretic mobility-shift assay) and ChIP (chromatin immunoprecipitation) assays show that Ixr1p binds to the IXR1 promoter both in vitro and in vivo. Ixr1p is also required for hypoxic repression of ROX1 and binds to its promoter. UPC2 deletion has opposite effects on IXR1 and ROX1 transcription during hypoxia. Ixr1p is also necessary for resistance to oxidative stress generated by H2O2. IXR1 expression is moderately activated by H2O2 and this induction is Yap1p-dependent. A model of IXR1 regulation as a relay for sensing different signals related to change in oxygen availability is proposed. In this model, transcriptional adaptation from aerobiosis to hypoxia depends on ROX1 and IXR1 cross-regulation.

摘要

酵母中的 Ixr1p 因能与顺铂等抗癌药物形成的链内交联 DNA 结合而被广泛研究。Ixr1p 也是厌氧/缺氧基因的转录调节剂,如编码应激反应细胞壁甘露糖蛋白的 SRP1/TIR1 和编码线粒体细胞色素 c 氧化酶 Vb 亚基的 COX5B。然而,控制 IXR1 表达的因素仍未被探索。本研究表明,IXR1 mRNA 水平受氧可用性控制,并在缺氧时增加。在需氧条件下,IXR1 的低水平表达通过 Rox1p 通过一般共阻遏复合物 Tup1-Ssn6 抑制来维持。在缺氧条件下,Ixr1p 本身对于完全表达 IXR1 是必需的。删除分析已经确定了 IXR1 启动子中负责这种正自动控制的区域(核苷酸 -557 至 -376)。EMSA(电泳迁移率变动分析)和 ChIP(染色质免疫沉淀)实验表明,Ixr1p 既在体外也在体内与 IXR1 启动子结合。Ixr1p 还需要缺氧抑制 ROX1 并与它的启动子结合。UPC2 的缺失对缺氧时 IXR1 和 ROX1 转录有相反的影响。Ixr1p 对于由 H2O2 产生的氧化应激的抵抗也是必需的。IXR1 的表达适度地被 H2O2 激活,这种诱导依赖于 Yap1p。提出了一个 IXR1 调节的模型,作为感知与氧可用性变化相关的不同信号的中继。在这个模型中,从需氧到缺氧的转录适应依赖于 ROX1 和 IXR1 的交叉调节。

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