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YgfZ 突变分析,一种与铁/硫簇代谢相关的依赖叶酸的蛋白。

Mutational analysis of YgfZ, a folate-dependent protein implicated in iron/sulphur cluster metabolism.

机构信息

Plant Molecular and Cellular Biology Program, University of Florida, Gainesville, USA.

出版信息

FEMS Microbiol Lett. 2012 Jan;326(2):168-72. doi: 10.1111/j.1574-6968.2011.02448.x. Epub 2011 Nov 18.

Abstract

Proteins of the YgfZ family occur in all domains of life and are characterized by the conserved dodecapeptide motif KGC[Y/F]-x-GQE-x(3) -[R/K]. YgfZ proteins are known to participate in assembly or repair of iron/sulphur clusters, and to require folate for biological activity, but their mechanism of action is unknown. To assess the importance of individual residues in the conserved motif, Escherichia coli Ygf Z was expressed from a plasmid in a ΔygfZ strain and subjected to alanine-scanning mutagenesis. The impacts on YgfZ functionality were evaluated by assays of growth and of the in vivo activity of the iron/sulphur enzyme MiaB, which modifies tRNA. By these criteria, the motif's tyrosine residue (Y229) had a detectable influence but only the cysteine residue (C228) was critical, for only the C228A mutant failed to complement the growth and MiaB activity phenotypes of the ΔygfZ strain. Immunoblots confirmed that the latter result was not simply because of a low level of the C228A mutant protein. Collectively, these data demonstrate a pivotal role for the Ygf Z motif's cysteine residue and a subsidiary one for the adjacent tyrosine, and help formulate a hypothesis about the folate requirement of Ygf Z proteins.

摘要

YgfZ 家族蛋白存在于所有生命领域,其特征是保守的十二肽基序 KGC[Y/F]-x-GQE-x(3) -[R/K]。已知 YgfZ 蛋白参与铁/硫簇的组装或修复,并需要叶酸才能发挥生物活性,但它们的作用机制尚不清楚。为了评估保守基序中单个残基的重要性,在ΔygfZ 菌株中,通过质粒表达了大肠杆菌 YgfZ,并进行了丙氨酸扫描诱变。通过生长和体内铁/硫酶 MiaB 的活性测定来评估对 YgfZ 功能的影响,MiaB 修饰 tRNA。根据这些标准,该基序的酪氨酸残基(Y229)有可检测的影响,但只有半胱氨酸残基(C228)是关键的,因为只有 C228A 突变体不能弥补ΔygfZ 菌株的生长和 MiaB 活性表型。免疫印迹证实,后一结果并非仅仅因为 C228A 突变体蛋白水平低。总的来说,这些数据表明 YgfZ 蛋白基序的半胱氨酸残基起着关键作用,而相邻的酪氨酸残基起着次要作用,并有助于形成关于 YgfZ 蛋白叶酸需求的假说。

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