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必需代谢酶MoeA的进化可塑性与功能重新利用

Evolutionary plasticity and functional repurposing of the essential metabolic enzyme MoeA.

作者信息

Megrian Daniela, Martinez Mariano, Alzari Pedro M, Wehenkel Anne Marie

机构信息

Institut Pasteur, CNRS UMR 3528, Université Paris Cité, Structural Microbiology Unit, F-75015 Paris, France.

Institut Pasteur de Montevideo, Bioinformatics Unit, 11200 Montevideo, Uruguay.

出版信息

bioRxiv. 2024 Jul 23:2024.07.23.604723. doi: 10.1101/2024.07.23.604723.

Abstract

MoeA, or gephyrin in higher eukaryotes, is crucial for molybdenum cofactor biosynthesis required in redox reactions. Gephyrin is a moonlighting protein also involved in postsynaptic receptor clustering, a feature thought to be a recent evolutionary trait. We showed previously that a repurposed copy of MoeA (Glp) is involved in bacterial cell division. To investigate how MoeA acquired multifunctionality, we used phylogenetic inference and protein structure analyses to understand the diversity and evolutionary history of MoeA. Glp-expressing Bacteria have at least two copies of the gene, and our analysis suggests that Glp has lost its enzymatic role. In Archaea we identified an ancestral duplication where one of the paralogs might bind tungsten instead of molybdenum. In eukaryotes, the acquisition of the moonlighting activity of gephyrin comprised three major events: first, MoeA was obtained from Bacteria by early eukaryotes, second, MogA was fused to the N-terminus of MoeA in the ancestor of opisthokonts, and finally, it acquired the function of anchoring GlyR receptors in neurons. Our results support the functional versatility and adaptive nature of the MoeA scaffold, which has been repurposed independently both in eukaryotes and bacteria to carry out analogous functions in network organization at the cell membrane.

摘要

MoeA,在高等真核生物中即桥连蛋白,对于氧化还原反应中所需的钼辅因子生物合成至关重要。桥连蛋白是一种具有多种功能的蛋白质,也参与突触后受体聚集,这一特性被认为是最近才出现的进化特征。我们之前表明,重新利用的MoeA拷贝(Glp)参与细菌细胞分裂。为了研究MoeA如何获得多功能性,我们使用系统发育推断和蛋白质结构分析来了解MoeA的多样性和进化历史。表达Glp的细菌至少有该基因的两个拷贝,我们的分析表明Glp已失去其酶促作用。在古菌中,我们发现了一次祖先基因复制事件,其中一个旁系同源物可能结合钨而非钼。在真核生物中,桥连蛋白获得兼职活性包括三个主要事件:首先,早期真核生物从细菌中获得MoeA;其次,在后生动物祖先中,MogA与MoeA的N端融合;最后,它获得了在神经元中锚定甘氨酸受体的功能。我们的结果支持了MoeA支架的功能多样性和适应性,它在真核生物和细菌中都被独立重新利用,以在细胞膜的网络组织中执行类似功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b99c/11291035/cdaf0a179fc6/nihpp-2024.07.23.604723v1-f0001.jpg

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