COG0523蛋白:从细菌到人类的过渡金属调控的G3E P-loop GTP水解酶的功能多样化家族。

IF 2.9 3区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Metallomics Pub Date : 2021-08-13 DOI:10.1093/mtomcs/mfab046
Katherine A Edmonds, Matthew R Jordan, David P Giedroc
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引用次数: 11

摘要

过渡金属稳态确保细胞和生物体获得足够的金属来满足细胞需求,同时排除任何多余的金属,以避免毒性。在细菌中,锌限制诱导一个或多个Zur(锌摄取抑制因子)调控的同源基团簇(COG) COG0523蛋白的表达。COG0523蛋白包含一个鲜为人知的G3E p环小gtpase亚家族,其中其他亚家族已知在钴胺素(CoII)和含NiII辅助因子的金属酶成熟过程中起金属伴侣作用。在这里,我们使用基因组酶学工具对8万多个序列进行了功能分析,这些序列与鲍曼不动杆菌ZigA(祖尔诱导的GTPase)、COG0523蛋白和候选锌金属伴侣蛋白进化相关。这些序列分离成不同的序列相似网络(SSN)簇,例如:ni - zir调控的和feiii -腈水合酶激活剂CxCC (C, Cys;包含COG0523蛋白(SSN集群1)、NiII-UreG(集群2,8)、CoII-CobW(集群4)和NiII-HypB(集群5)的5个大集群占所有序列的约25%,包括集群3,其中包含唯一结构表征的COG0523蛋白、大肠杆菌YjiA和许多未表征的真核COG0523蛋白。我们还发现,在ni饥饿条件下促进放线菌核糖体冬眠的分枝杆菌特异性蛋白Y (Mpy)募集因子(Mrf)分离成第五个SSN簇(簇17)。Mrf是一种COG0523类似物,缺乏所有gtp结合决定因子以及在含有cxcc的COG0523蛋白中发现的zni -协调Cys。在此基础上,我们讨论了COG0523蛋白作为广泛的营养胁迫的细胞报告者的新观点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

COG0523 proteins: a functionally diverse family of transition metal-regulated G3E P-loop GTP hydrolases from bacteria to man.

COG0523 proteins: a functionally diverse family of transition metal-regulated G3E P-loop GTP hydrolases from bacteria to man.

COG0523 proteins: a functionally diverse family of transition metal-regulated G3E P-loop GTP hydrolases from bacteria to man.

COG0523 proteins: a functionally diverse family of transition metal-regulated G3E P-loop GTP hydrolases from bacteria to man.

Transition metal homeostasis ensures that cells and organisms obtain sufficient metal to meet cellular demand while dispensing with any excess so as to avoid toxicity. In bacteria, zinc restriction induces the expression of one or more Zur (zinc-uptake repressor)-regulated Cluster of Orthologous Groups (COG) COG0523 proteins. COG0523 proteins encompass a poorly understood sub-family of G3E P-loop small GTPases, others of which are known to function as metallochaperones in the maturation of cobalamin (CoII) and NiII cofactor-containing metalloenzymes. Here, we use genomic enzymology tools to functionally analyse over 80 000 sequences that are evolutionarily related to Acinetobacter baumannii ZigA (Zur-inducible GTPase), a COG0523 protein and candidate zinc metallochaperone. These sequences segregate into distinct sequence similarity network (SSN) clusters, exemplified by the ZnII-Zur-regulated and FeIII-nitrile hydratase activator CxCC (C, Cys; X, any amino acid)-containing COG0523 proteins (SSN cluster 1), NiII-UreG (clusters 2, 8), CoII-CobW (cluster 4), and NiII-HypB (cluster 5). A total of five large clusters that comprise ≈ 25% of all sequences, including cluster 3 which harbors the only structurally characterized COG0523 protein, Escherichia coli YjiA, and many uncharacterized eukaryotic COG0523 proteins. We also establish that mycobacterial-specific protein Y (Mpy) recruitment factor (Mrf), which promotes ribosome hibernation in actinomycetes under conditions of ZnII starvation, segregates into a fifth SSN cluster (cluster 17). Mrf is a COG0523 paralog that lacks all GTP-binding determinants as well as the ZnII-coordinating Cys found in CxCC-containing COG0523 proteins. On the basis of this analysis, we discuss new perspectives on the COG0523 proteins as cellular reporters of widespread nutrient stress induced by ZnII limitation.

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来源期刊
Metallomics
Metallomics 生物-生化与分子生物学
CiteScore
7.00
自引率
5.90%
发文量
87
审稿时长
1 months
期刊介绍: Global approaches to metals in the biosciences
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