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真核生物叶酸生物合成途径中复杂的基因裂变模式。

Complex patterns of gene fission in the eukaryotic folate biosynthesis pathway.

作者信息

Maguire Finlay, Henriquez Fiona L, Leonard Guy, Dacks Joel B, Brown Matthew W, Richards Thomas A

机构信息

Department of Life Sciences, Natural History Museum, London, United Kingdom.

Infection and Microbiology Research Group, Institute of Biomedical and Environmental Health Research, School of Science, University of the West of Scotland, Paisley, Renfrewshire, United Kingdom.

出版信息

Genome Biol Evol. 2014 Sep 23;6(10):2709-20. doi: 10.1093/gbe/evu213.

Abstract

Shared derived genomic characters can be useful for polarizing phylogenetic relationships, for example, gene fusions have been used to identify deep-branching relationships in the eukaryotes. Here, we report the evolutionary analysis of a three-gene fusion of folB, folK, and folP, which encode enzymes that catalyze consecutive steps in de novo folate biosynthesis. The folK-folP fusion was found across the eukaryotes and a sparse collection of prokaryotes. This suggests an ancient derivation with a number of gene losses in the eukaryotes potentially as a consequence of adaptation to heterotrophic lifestyles. In contrast, the folB-folK-folP gene is specific to a mosaic collection of Amorphea taxa (a group encompassing: Amoebozoa, Apusomonadida, Breviatea, and Opisthokonta). Next, we investigated the stability of this character. We identified numerous gene losses and a total of nine gene fission events, either by break up of an open reading frame (four events identified) or loss of a component domain (five events identified). This indicates that this three gene fusion is highly labile. These data are consistent with a growing body of data indicating gene fission events occur at high relative rates. Accounting for these sources of homoplasy, our data suggest that the folB-folK-folP gene fusion was present in the last common ancestor of Amoebozoa and Opisthokonta but absent in the Metazoa including the human genome. Comparative genomic data of these genes provides an important resource for designing therapeutic strategies targeting the de novo folate biosynthesis pathway of a variety of eukaryotic pathogens such as Acanthamoeba castellanii.

摘要

共享的衍生基因组特征可用于确定系统发育关系的极性,例如,基因融合已被用于识别真核生物中的深层分支关系。在此,我们报告了folB、folK和folP三个基因融合的进化分析,这三个基因编码催化从头合成叶酸连续步骤的酶。在真核生物和少量原核生物中发现了folK-folP融合。这表明其起源古老,真核生物中存在一些基因丢失现象,这可能是适应异养生活方式的结果。相比之下,folB-folK-folP基因特定于变形虫类群的一个镶嵌集合(该类群包括:变形虫门、无鞭毛门、短膜虫纲和后鞭毛生物)。接下来,我们研究了这一特征的稳定性。我们识别出了大量的基因丢失以及总共九次基因分裂事件,这些事件要么是由开放阅读框的断裂(识别出四次事件)引起,要么是由一个组成结构域的丢失(识别出五次事件)引起。这表明这种三基因融合非常不稳定。这些数据与越来越多表明基因分裂事件以较高相对速率发生的数据相一致。考虑到这些平行进化的来源,我们的数据表明folB-folK-folP基因融合存在于变形虫门和后鞭毛生物的最后共同祖先中,但在包括人类基因组在内的后生动物中不存在。这些基因的比较基因组数据为设计针对多种真核病原体(如卡氏棘阿米巴)从头合成叶酸途径的治疗策略提供了重要资源。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1fb3/4224340/6714c3d5c6c2/evu213f1p.jpg

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