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Structure determination of the HgcAB complex using metagenome sequence data: insights into microbial mercury methylation

机译:使用Metagenome序列数据的HGCAB复合物的结构测定:洞察微生物汞甲基化

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Bacteria and archaea possessing the hgcAB gene pair methylate inorganic mercury (Hg) to form highly toxic methylmercury. HgcA consists of a corrinoid binding domain and a transmembrane domain, and HgcB is a dicluster ferredoxin. However, their detailed structure and function have not been thoroughly characterized. We modeled the HgcAB complex by combining metagenome sequence data mining, coevolution analysis, and Rosetta structure calculations. In addition, we overexpressed HgcA and HgcB in Escherichia coli, confirmed spectroscopically that they bind cobalamin and [4Fe-4S] clusters, respectively, and incorporated these cofactors into the structural model. Surprisingly, the two domains of HgcA do not interact with each other, but HgcB forms extensive contacts with both domains. The model suggests that conserved cysteines in HgcB are involved in shuttling HgII, methylmercury, or both. These findings refine our understanding of the mechanism of Hg methylation and expand the known repertoire of corrinoid methyltransferases in nature. Connor J. Cooper et al. expressed HgcA and HgcB in Escherichia coli and modeled the structure of the HgcAB complex by combining metagenome sequence data, coevolution analysis, and ab initio structure calculations. This study provides insights into the biochemical mechanism of mercury (Hg) methylation.
机译:具有Hgcab基因对甲酸甲酯无机汞(HG)的细菌和古痤疮形成高度毒性甲基汞。 HGCA由甲状状结合结构域和跨膜结构域组成,HGCB是Dicluster Ferredoxin。但是,它们的详细结构和功能尚未完全表征。我们通过组合梅塔群序列数据挖掘,共同化分析和Rosetta结构计算来建模HGCAB复合物。此外,我们在大肠杆菌中过表达HGCA和HGCB,在光谱上确认它们分别与钴胺蛋白和[4FE-4S]簇结合,并将这些辅助粘液掺入结构模型中。令人惊讶的是,HGCA的两个域不会相互作用,但HGCB与两个域形成广泛的接触。该模型表明HGCB中的保守半胱氨酸涉及穿梭HGII,甲基汞或两者。这些发现优化了我们对HG甲基化机制的理解,并在自然中展开了甲甲基转移酶的已知曲目。 Connor J. Cooper等人。在大肠杆菌中表达HGCA和HGCB,并通过组合梅塔群序列数据,共识别分析和AB初始结构计算来建模HGCAB复合物的结构。本研究为汞(Hg)甲基化的生化机制提供了见解。

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