首页> 外文期刊>Toxicological sciences: An official journal of the Society of Toxicology >Identification of genes involved in the toxic response of Saccharomyces cerevisiae against iron and copper overload by parallel analysis of deletion mutants.
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Identification of genes involved in the toxic response of Saccharomyces cerevisiae against iron and copper overload by parallel analysis of deletion mutants.

机译:通过缺失突变体的平行分析,鉴定涉及酿酒酵母对铁和铜超载毒性反应的基因。

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Iron and copper are essential nutrients for life as they are required for the function of many proteins but can be toxic if present in excess. Accumulation of these metals in the human body as a consequence of overload disorders and/or high environmental exposures has detrimental effects on health. The budding yeast Saccharomyces cerevisiae is an accepted cellular model for iron and copper metabolism in humans primarily because of the high degree of conservation between pathways and proteins involved. Here we report a systematic screen using yeast deletion mutants to identify genes involved in the toxic response to growth-inhibitory concentrations of iron and copper sulfate. We aimed to understand the cellular responses to toxic concentrations of these two metals by analyzing the different subnetworks and biological processes significantly enriched with these genes. Our results indicate the presence of two different detoxification pathways for iron and copper that converge toward the vacuole. The product of several of the identified genes in these pathways form molecular complexes that are conserved in mammals and include the retromer, endosomal sorting complex required for transport (ESCRT) and AP-3 complexes, suggesting that the mechanisms involved can be extrapolated to humans. Our data also suggest a disruption in ion homeostasis and, in particular, of iron after copper exposure. Moreover, the identification of treatment-specific genes associated with biological processes such as DNA double-strand break repair for iron and tryptophan biosynthesis for copper suggests differences in the mechanisms by which these two metals are toxic at high concentrations.
机译:铁和铜是生命中必不可少的营养素,因为它们是许多蛋白质功能所必需的,但如果铁和铜的含量过多,则可能具有毒性。过载疾病和/或高环境暴露的结果是这些金属在人体中的积累会对健康产生不利影响。出芽的酿酒酵母是人类公认的用于铁和铜代谢的细胞模型,这主要是由于途径和涉及的蛋白质之间的高度保守性。在这里,我们报告了使用酵母缺失突变体进行系统的筛选,以鉴定参与对生长抑制浓度的铁和硫酸铜的毒性反应的基因。我们旨在通过分析不同的子网络和明显富集这些基因的生物过程,来了解细胞对这两种金属的毒性浓度的反应。我们的结果表明,铁和铜有两种不同的排毒途径,它们都向液泡会聚。这些途径中几个已鉴定基因的产物形成了在哺乳动物中保守的分子复合物,包括逆转录,转运所需的内体分选复合物(ESCRT)和AP-3复合物,表明所涉及的机制可以推断给人类。我们的数据还表明,离子稳态,尤其是铜暴露后的铁离子稳态被破坏。此外,与生物过程相关的治疗特异性基因的鉴定,如铁的DNA双链断裂修复和铜的色氨酸生物合成,提示这两种金属在高浓度下有毒的机理不同。

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