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拟菌病毒揭示了在真核生物、细菌、病毒和质粒中具有散在分布的 Mre11/Rad50 融合蛋白。

Mimivirus reveals Mre11/Rad50 fusion proteins with a sporadic distribution in eukaryotes, bacteria, viruses and plasmids.

机构信息

Structural and Genomic Information Laboratory, CNRS-UPR 2589, Aix-Marseille University, Mediterranean Institute of Microbiology, 163 Avenue de Luminy, Case 934, 13288 Marseille Cedex 9, France.

出版信息

Virol J. 2011 Sep 7;8:427. doi: 10.1186/1743-422X-8-427.

Abstract

BACKGROUND

The Mre11/Rad50 complex and the homologous SbcD/SbcC complex in bacteria play crucial roles in the metabolism of DNA double-strand breaks, including DNA repair, genome replication, homologous recombination and non-homologous end-joining in cellular life forms and viruses. Here we investigated the amino acid sequence of the Mimivirus R555 gene product, originally annotated as a Rad50 homolog, and later shown to have close homologs in marine microbial metagenomes.

RESULTS

Our bioinformatics analysis revealed that R555 protein sequence is constituted from the fusion of an N-terminal Mre11-like domain with a C-terminal Rad50-like domain. A systematic database search revealed twelve additional cases of Mre11/Rad50 (or SbcD/SbcC) fusions in a wide variety of unrelated organisms including unicellular and multicellular eukaryotes, the megaplasmid of a bacterium associated to deep-sea hydrothermal vents (Deferribacter desulfuricans) and the plasmid of Clostridium kluyveri. We also showed that R555 homologs are abundant in the metagenomes from different aquatic environments and that they most likely belong to aquatic viruses. The observed phyletic distribution of these fusion proteins suggests their recurrent creation and lateral gene transfers across organisms.

CONCLUSIONS

The existence of the fused version of protein sequences is consistent with known functional interactions between Mre11 and Rad50, and the gene fusion probably enhanced the opportunity for lateral transfer. The abundance of the Mre11/Rad50 fusion genes in viral metagenomes and their sporadic phyletic distribution in cellular organisms suggest that viruses, plasmids and transposons played a crucial role in the formation of the fusion proteins and their propagation into cellular genomes.

摘要

背景

Mre11/Rad50 复合物和细菌中的同源 SbcD/SbcC 复合物在 DNA 双链断裂的代谢中发挥着至关重要的作用,包括细胞生命形式和病毒中的 DNA 修复、基因组复制、同源重组和非同源末端连接。在这里,我们研究了 Mimivirus R555 基因产物的氨基酸序列,该基因产物最初被注释为 Rad50 同源物,后来在海洋微生物宏基因组中发现了其密切的同源物。

结果

我们的生物信息学分析表明,R555 蛋白序列由 N 端 Mre11 样结构域与 C 端 Rad50 样结构域融合而成。系统的数据库搜索显示,在包括单细胞和多细胞真核生物在内的各种无关生物体中,有 12 个额外的 Mre11/Rad50(或 SbcD/SbcC)融合体的例子,包括与深海热液喷口相关的细菌的巨质粒(Deferribacter desulfuricans)和 Clostridium kluyveri 的质粒。我们还表明,R555 同源物在来自不同水生环境的宏基因组中大量存在,它们很可能属于水生病毒。这些融合蛋白的观察到的系统发育分布表明它们在生物体之间经常发生创造和横向基因转移。

结论

融合蛋白序列的存在与 Mre11 和 Rad50 之间已知的功能相互作用一致,并且基因融合可能增强了横向转移的机会。在病毒宏基因组中大量存在的 Mre11/Rad50 融合基因及其在细胞生物中的分散系统发育分布表明,病毒、质粒和转座子在融合蛋白的形成及其在细胞基因组中的传播中发挥了关键作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f1be/3175470/ab99a5529e8c/1743-422X-8-427-1.jpg

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