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囊泡虫类及其他微生物真核生物中胞质铁硫簇组装机制的进化

Evolution of the cytosolic iron-sulfur cluster assembly machinery in Blastocystis species and other microbial eukaryotes.

作者信息

Tsaousis Anastasios D, Gentekaki Eleni, Eme Laura, Gaston Daniel, Roger Andrew J

机构信息

Centre for Comparative Genomics and Evolutionary Bioinformatics, Dalhousie University, Department of Biochemistry and Molecular Biology, Halifax, Nova Scotia, Canada.

出版信息

Eukaryot Cell. 2014 Jan;13(1):143-53. doi: 10.1128/EC.00158-13. Epub 2013 Nov 15.

Abstract

The cytosolic iron/sulfur cluster assembly (CIA) machinery is responsible for the assembly of cytosolic and nuclear iron/sulfur clusters, cofactors that are vital for all living cells. This machinery is uniquely found in eukaryotes and consists of at least eight proteins in opisthokont lineages, such as animals and fungi. We sought to identify and characterize homologues of the CIA system proteins in the anaerobic stramenopile parasite Blastocystis sp. strain NandII. We identified transcripts encoding six of the components-Cia1, Cia2, MMS19, Nbp35, Nar1, and a putative Tah18-and showed using immunofluorescence microscopy, immunoelectron microscopy, and subcellular fractionation that the last three of them localized to the cytoplasm of the cell. We then used comparative genomic and phylogenetic approaches to investigate the evolutionary history of these proteins. While most Blastocystis homologues branch with their eukaryotic counterparts, the putative Blastocystis Tah18 seems to have a separate evolutionary origin and therefore possibly a different function. Furthermore, our phylogenomic analyses revealed that all eight CIA components described in opisthokonts originated before the diversification of extant eukaryotic lineages and were likely already present in the last eukaryotic common ancestor (LECA). The Nbp35, Nar1 Cia1, and Cia2 proteins have been conserved during the subsequent evolutionary diversification of eukaryotes and are present in virtually all extant lineages, whereas the other CIA proteins have patchy phylogenetic distributions. Cia2 appears to be homologous to SufT, a component of the prokaryotic sulfur utilization factors (SUF) system, making this the first reported evolutionary link between the CIA and any other Fe/S biogenesis pathway. All of our results suggest that the CIA machinery is an ubiquitous biosynthetic pathway in eukaryotes, but its apparent plasticity in composition raises questions regarding how it functions in nonmodel organisms and how it interfaces with various iron/sulfur cluster systems (i.e., the iron/sulfur cluster, nitrogen fixation, and/or SUF system) found in eukaryotic cells.

摘要

胞质铁硫簇组装(CIA)机制负责胞质和细胞核中铁硫簇的组装,这些辅因子对所有活细胞都至关重要。这种机制仅在真核生物中发现,在动物和真菌等后鞭毛生物谱系中至少由八种蛋白质组成。我们试图在厌氧不等鞭毛寄生虫纳氏芽囊原虫菌株NandII中鉴定并表征CIA系统蛋白的同源物。我们鉴定出了编码六种组分的转录本——Cia1、Cia2、MMS19、Nbp35、Nar1和一种假定的Tah18——并通过免疫荧光显微镜、免疫电子显微镜和亚细胞分级分离表明,其中最后三种定位于细胞的细胞质中。然后,我们使用比较基因组学和系统发育方法来研究这些蛋白质的进化历史。虽然大多数芽囊原虫同源物与其真核对应物分支,但假定的芽囊原虫Tah18似乎有一个独立的进化起源,因此可能具有不同的功能。此外,我们的系统基因组分析表明,后鞭毛生物中描述的所有八种CIA组分在现存真核生物谱系多样化之前就已起源,并且可能已经存在于最后一个真核生物共同祖先(LECA)中。Nbp35、Nar1、Cia1和Cia2蛋白在真核生物随后的进化多样化过程中一直保守,几乎存在于所有现存谱系中,而其他CIA蛋白的系统发育分布则不连续。Cia2似乎与原核生物硫利用因子(SUF)系统的一个组分SufT同源,这使得这成为首次报道的CIA与任何其他铁硫生物合成途径之间的进化联系。我们所有的结果表明,CIA机制是真核生物中一种普遍存在的生物合成途径,但它在组成上的明显可塑性引发了关于它在非模式生物中如何发挥作用以及它如何与真核细胞中发现的各种铁硫簇系统(即铁硫簇、固氮和/或SUF系统)相互作用的问题。

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