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疟原虫毒力基因间的重组事件与形成G-四链体的DNA基序有关。

Recombination events among virulence genes in malaria parasites are associated with G-quadruplex-forming DNA motifs.

作者信息

Stanton Adam, Harris Lynne M, Graham Gemma, Merrick Catherine J

机构信息

School of Computing and Mathematics, Faculty of Natural Sciences, Keele University, Keele, Staffordshire, ST55BG, UK.

Centre for Applied Entomology and Parasitology, Faculty of Natural Sciences, Keele University, Keele, Staffordshire, ST55BG, UK.

出版信息

BMC Genomics. 2016 Nov 3;17(1):859. doi: 10.1186/s12864-016-3183-3.

Abstract

BACKGROUND

Malaria parasites of the genus Plasmodium possess large hyper-variable families of antigen-encoding genes. These are often variantly-expressed and are major virulence factors for immune evasion and the maintenance of chronic infections. Recombination and diversification of these gene families occurs readily, and may be promoted by G-quadruplex (G4) DNA motifs within and close to the variant genes. G4s have been shown to cause replication fork stalling, DNA breakage and recombination in model systems, but these motifs remain largely unstudied in Plasmodium.

RESULTS

We examined the nature and distribution of putative G4-forming sequences in multiple Plasmodium genomes, finding that their co-distribution with variant gene families is conserved across different Plasmodium species that have different types of variant gene families. In P. falciparum, where a large set of recombination events that occurred over time in cultured parasites has been mapped, we found a strong spatial association between these recombination events and putative G4-forming sequences. Finally, we searched Plasmodium genomes for the three classes of helicase that can unwind G4s: Plasmodium spp. have no identifiable homologue of the highly efficient G4 helicase PIF1, but they do encode two putative RecQ helicases and one homologue of the RAD3-family helicase FANCJ.

CONCLUSIONS

Our analyses, conducted at the whole-genome level in multiple species of Plasmodium, support the concept that G4s are likely to be involved in recombination and diversification of antigen-encoding gene families in this important protozoan pathogen.

摘要

背景

疟原虫属的疟原虫拥有大量高度可变的抗原编码基因家族。这些基因通常以可变方式表达,是免疫逃避和维持慢性感染的主要毒力因子。这些基因家族的重组和多样化很容易发生,并且可能由可变基因内部和附近的G-四链体(G4)DNA基序促进。在模型系统中,G4已被证明会导致复制叉停滞、DNA断裂和重组,但这些基序在疟原虫中仍基本未被研究。

结果

我们研究了多个疟原虫基因组中假定的G4形成序列的性质和分布,发现它们与可变基因家族的共分布在具有不同类型可变基因家族的不同疟原虫物种中是保守的。在恶性疟原虫中,已经绘制了培养寄生虫中随时间发生的大量重组事件,我们发现这些重组事件与假定的G4形成序列之间存在很强的空间关联。最后,我们在疟原虫基因组中搜索了可以解开G4的三类解旋酶:疟原虫属没有高效G4解旋酶PIF1的可识别同源物,但它们确实编码两种假定的RecQ解旋酶和一种RAD3家族解旋酶FANCJ的同源物。

结论

我们在多个疟原虫物种的全基因组水平上进行的分析支持这样一种概念,即G4可能参与这种重要原生动物病原体中抗原编码基因家族的重组和多样化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f053/5093961/64667f9de279/12864_2016_3183_Fig1_HTML.jpg

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