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一种用于研究酿酒酵母铁调节子的铜积累化学增强剂。

A chemical potentiator of copper-accumulation used to investigate the iron-regulons of Saccharomyces cerevisiae.

作者信息

Foster Andrew W, Dainty Samantha J, Patterson Carl J, Pohl Ehmke, Blackburn Hannah, Wilson Clare, Hess Corinna R, Rutherford Julian C, Quaranta Laura, Corran Andy, Robinson Nigel J

机构信息

Department of Chemistry, School of Biological and Biomedical Sciences, Durham University, Durham, DH1 3LE, UK.

出版信息

Mol Microbiol. 2014 Jul;93(2):317-30. doi: 10.1111/mmi.12661. Epub 2014 Jun 15.

Abstract

The extreme resistance of Saccharomyces cerevisiae to copper is overcome by 2-(6-benzyl-2-pyridyl)quinazoline (BPQ), providing a chemical-biology tool which has been exploited in two lines of discovery. First, BPQ is shown to form a red (BPQ)2 Cu(I) complex and promote Ctr1-independent copper-accumulation in whole cells and in mitochondria isolated from treated cells. Multiple phenotypes, including loss of aconitase activity, are consistent with copper-BPQ mediated damage to mitochondrial iron-sulphur clusters. Thus, a biochemical basis of copper-toxicity in S. cerevisiae is analogous to other organisms. Second, iron regulons controlled by Aft1/2, Cth2 and Yap5 that respond to mitochondrial iron-sulphur cluster status are modulated by copper-BPQ causing iron hyper-accumulation via upregulated iron-import. Comparison of copper-BPQ treated, untreated and copper-only treated wild-type and fra2Δ by RNA-seq has uncovered a new candidate Aft1 target-gene (LSO1) and paralogous non-target (LSO2), plus nine putative Cth2 target-transcripts. Two lines of evidence confirm that Fra2 dominates basal repression of the Aft1/2 regulons in iron-replete cultures. Fra2-independent control of these regulons is also observed but CTH2 itself appears to be atypically Fra2-dependent. However, control of Cth2-target transcripts which is independent of CTH2 transcript abundance or of Fra2, is also quantified. Use of copper-BPQ supports a substantial contribution of metabolite repression to iron-regulation.

摘要

酿酒酵母对铜的极端抗性可被2-(6-苄基-2-吡啶基)喹唑啉(BPQ)克服,这提供了一种化学生物学工具,已被用于两项发现研究中。首先,BPQ被证明能形成红色的(BPQ)2 Cu(I)复合物,并促进全细胞以及从处理过的细胞中分离出的线粒体中不依赖Ctr1的铜积累。多种表型,包括乌头酸酶活性丧失,都与铜-BPQ介导的线粒体铁硫簇损伤一致。因此,酿酒酵母中铜毒性的生化基础与其他生物体类似。其次,由Aft1/2、Cth2和Yap5控制的、对线粒体铁硫簇状态作出反应的铁调节子受到铜-BPQ的调节,通过上调铁的输入导致铁过度积累。通过RNA测序比较铜-BPQ处理、未处理以及仅用铜处理的野生型和fra2Δ,发现了一个新的Aft1靶基因候选基因(LSO1)和同源非靶基因(LSO2),以及9个假定的Cth2靶转录本。有两条证据证实,在铁充足的培养物中,Fra2主导对Aft1/2调节子的基础抑制。也观察到这些调节子的Fra2非依赖性控制,但CTH2本身似乎非典型地依赖Fra2。然而,也对独立于CTH2转录本丰度或Fra2的Cth2靶转录本的控制进行了定量。铜-BPQ的使用支持了代谢物阻遏对铁调节的重大贡献。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9fd6/4149784/682186c90cd1/mmi0093-0317-f1.jpg

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