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Response to Arsenate Treatment in Schizosaccharomyces pombe and the Role of Its Arsenate Reductase Activity

机译:响应砷治疗裂殖酵母及其砷酸还原酶活性的作用

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摘要

Arsenic toxicity has been studied for a long time due to its effects in humans. Although epidemiological studies have demonstrated multiple effects in human physiology, there are many open questions about the cellular targets and the mechanisms of response to arsenic. Using the fission yeast Schizosaccharomyces pombe as model system, we have been able to demonstrate a strong activation of the MAPK Spc1/Sty1 in response to arsenate. This activation is dependent on Wis1 activation and Pyp2 phosphatase inactivation. Using arsenic speciation analysis we have also demonstrated the previously unknown capacity of S. pombe cells to reduce As (V) to As (III). Genetic analysis of several fission yeast mutants point towards the cell cycle phosphatase Cdc25 as a possible candidate to carry out this arsenate reductase activity. We propose that arsenate reduction and intracellular accumulation of arsenite are the key mechanisms of arsenate tolerance in fission yeast.
机译:由于砷对人体的影响,已经对其进行了长期的研究。尽管流行病学研究已经证明了对人类生理的多种影响,但是关于细胞靶标和对砷的反应机制仍有许多悬而未决的问题。使用裂变酵母粟酒裂殖酵母作为模型系统,我们已经能够证明MAPK Spc1 / Sty1对砷酸有很强的激活作用。此激活取决于Wis1激活和Pyp2磷酸酶失活。使用砷形态分析,我们还证明了粟酒裂殖酵母细胞以前未知的将As(V)还原为As(III)的能力。几个裂变酵母突变体的遗传分析指向细胞周期磷酸酶Cdc25,作为进行这种砷酸还原酶活性的可能候选者。我们提出砷减少和砷在胞内积累是裂殖酵母中砷耐受的关键机制。

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