首页> 外文期刊>Dalton transactions: An international journal of inorganic chemistry >Iron binding activity is essential for the function of IscA in iron-sulphur cluster biogenesis
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Iron binding activity is essential for the function of IscA in iron-sulphur cluster biogenesis

机译:铁结合活性对于IscA在铁-硫簇生物发生中的功能至关重要

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摘要

Iron-sulphur cluster biogenesis requires coordinated delivery of iron and sulphur to scaffold proteins, followed by transfer of the assembled clusters from scaffold proteins to target proteins. This complex process is accomplished by a group of dedicated iron-sulphur cluster assembly proteins that are conserved from bacteria to humans. While sulphur in iron-sulphur clusters is provided by l-cysteine via cysteine desulfurase, the iron donor(s) for iron-sulphur cluster assembly remains largely elusive. Here we report that among the primary iron-sulphur cluster assembly proteins, IscA has a unique and strong binding activity for mononuclear iron in vitro and in vivo. Furthermore, the ferric iron centre tightly bound in IscA can be readily extruded by l-cysteine, followed by reduction to ferrous iron for iron-sulphur cluster biogenesis. Substitution of the highly conserved residue tyrosine 40 with phenylalanine (Y40F) in IscA results in a mutant protein that has a diminished iron binding affinity but retains the iron-sulphur cluster binding activity. Genetic complementation studies show that the IscA Y40F mutant is inactive in vivo, suggesting that the iron binding activity is essential for the function of IscA in iron-sulphur cluster biogenesis.
机译:铁-硫团簇的生物发生需要铁和硫的协同递送至支架蛋白,然后将组装好的簇从支架蛋白转移至靶蛋白。这个复杂的过程是通过一组专用的铁-硫簇装配蛋白完成的,这些蛋白从细菌到人类都是保守的。尽管L-半胱氨酸通过半胱氨酸脱硫酶提供了铁-硫簇中的硫,但铁-硫簇组装中的铁供体仍然难以捉摸。在这里我们报告,在主要的铁-硫簇装配蛋白中,IscA在体外和体内对单核铁具有独特而强大的结合活性。此外,紧密结合在IscA中的三价铁中心可以很容易地被L-半胱氨酸挤压,然后还原成亚铁,从而形成铁-硫团簇。 IscA中高度保守的酪氨酸40残基被苯丙氨酸(Y40F)取代后,突变蛋白的铁结合亲和力降低,但仍保留了铁-硫簇的结合活性。遗传互补研究表明,IscA Y40F突变体在体内无活性,这表明铁结合活性对于IscA在铁-硫簇生物发生中的功能至关重要。

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