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通过 Thermoanaerobacter tengcongensis 中与丙酮酸-铁氧还蛋白氧化还原酶的相互作用调节醇脱氢酶的酶活性。

Regulation of enzyme activity of alcohol dehydrogenase through its interactions with pyruvate-ferredoxin oxidoreductase in Thermoanaerobacter tengcongensis.

机构信息

Beijing Institute of Genomics, Chinese Academy of Sciences, China.

出版信息

Biochem Biophys Res Commun. 2012 Jan 20;417(3):1018-23. doi: 10.1016/j.bbrc.2011.12.083. Epub 2011 Dec 26.

DOI:10.1016/j.bbrc.2011.12.083
PMID:22222371
Abstract

Alcohol dehydrogenases (ADHs) from thermophilic microorganisms are interesting enzymes that have their potential applications in biotechnology and potentially provide insight into the mechanisms of action of thermo-tolerant proteins. The molecular mechanisms of ADHs under thermal stress in vivo have yet to be explored. Herein, we employed a proteomic strategy to survey the possible interactions of secondary-ADH (2-ADH) with other proteins in Thermoanaerobacter tengcongensis (T. tengcongensis) cultured at 75°C and found that 2-ADH, pyruvate-ferredoxin oxidoreductase (PFOR) and several glycolytic enzymes coexisted in a protein complex. Using anion exchange chromatography, the elution profile indicated that the native 2-ADH was present in two forms, PFOR-bound and PFOR-free. Immuno-precipitation and pull down analysis further validated the interactions between 2-ADH and PFOR. The kinetic behaviours of 2-ADH either in the recombinant or native form were evaluated with different substrates. The enzyme activity of 2-ADH was inhibited in a non-competitive mode by PFOR, implying the interaction of 2-ADH and PFOR negatively regulated alcohol formation. In T. tengcongensis, PFOR is an enzyme complex located at the upstream of 2-ADH in the alcohol generation pathway. These findings, therefore, offered a plausible mechanism for how alcohol metabolism is regulated by hetero-interactions between 2-ADH and PFOR, especially in anaerobic thermophiles.

摘要

嗜热微生物中的醇脱氢酶(ADHs)是一类有趣的酶,它们在生物技术中有潜在的应用价值,并可能为耐热蛋白的作用机制提供深入的了解。ADH 在体内热应激下的分子机制尚未被探索。在此,我们采用蛋白质组学策略来研究嗜热厌氧菌(T. tengcongensis)中 2-ADH 与其他蛋白质的可能相互作用,这些菌在 75°C 下培养,结果发现 2-ADH、丙酮酸铁氧还蛋白氧化还原酶(PFOR)和几种糖酵解酶存在于一个蛋白质复合物中。通过阴离子交换层析,洗脱图谱表明天然 2-ADH 以两种形式存在,与 PFOR 结合和游离形式。免疫沉淀和下拉分析进一步验证了 2-ADH 和 PFOR 之间的相互作用。使用不同的底物评估了重组和天然形式的 2-ADH 的动力学行为。2-ADH 的酶活性以非竞争性方式被 PFOR 抑制,这表明 2-ADH 和 PFOR 的相互作用负调控了酒精的形成。在 T. tengcongensis 中,PFOR 是位于 2-ADH 酒精生成途径上游的酶复合物。因此,这些发现为 2-ADH 和 PFOR 之间的异质相互作用如何调节酒精代谢提供了一个合理的机制,特别是在厌氧嗜热菌中。

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