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隐匿性黑猩猩疟原虫物种的基因组揭示了导致人类疟疾的关键进化事件。

Genomes of cryptic chimpanzee Plasmodium species reveal key evolutionary events leading to human malaria.

作者信息

Sundararaman Sesh A, Plenderleith Lindsey J, Liu Weimin, Loy Dorothy E, Learn Gerald H, Li Yingying, Shaw Katharina S, Ayouba Ahidjo, Peeters Martine, Speede Sheri, Shaw George M, Bushman Frederic D, Brisson Dustin, Rayner Julian C, Sharp Paul M, Hahn Beatrice H

机构信息

Department of Medicine, University of Pennsylvania, Philadelphia, 19104 Pennsylvania, USA.

Department of Microbiology, University of Pennsylvania, Philadelphia, 19104 Pennsylvania, USA.

出版信息

Nat Commun. 2016 Mar 22;7:11078. doi: 10.1038/ncomms11078.

Abstract

African apes harbour at least six Plasmodium species of the subgenus Laverania, one of which gave rise to human Plasmodium falciparum. Here we use a selective amplification strategy to sequence the genome of chimpanzee parasites classified as Plasmodium reichenowi and Plasmodium gaboni based on the subgenomic fragments. Genome-wide analyses show that these parasites indeed represent distinct species, with no evidence of cross-species mating. Both P. reichenowi and P. gaboni are 10-fold more diverse than P. falciparum, indicating a very recent origin of the human parasite. We also find a remarkable Laverania-specific expansion of a multigene family involved in erythrocyte remodelling, and show that a short region on chromosome 4, which encodes two essential invasion genes, was horizontally transferred into a recent P. falciparum ancestor. Our results validate the selective amplification strategy for characterizing cryptic pathogen species, and reveal evolutionary events that likely predisposed the precursor of P. falciparum to colonize humans.

摘要

非洲猿类携带着至少六种疟原虫亚属(Laverania)的疟原虫,其中一种演化出了人类疟原虫恶性疟原虫(Plasmodium falciparum)。在此,我们采用一种选择性扩增策略,对基于亚基因组片段被归类为莱氏疟原虫(Plasmodium reichenowi)和加蓬疟原虫(Plasmodium gaboni)的黑猩猩疟原虫基因组进行测序。全基因组分析表明,这些疟原虫确实代表不同的物种,没有跨物种交配的证据。莱氏疟原虫和加蓬疟原虫的多样性均比恶性疟原虫高10倍,这表明人类疟原虫起源非常晚近。我们还发现了一个参与红细胞重塑的多基因家族在疟原虫亚属中显著扩张,并表明4号染色体上一个编码两个关键入侵基因的短区域被水平转移到了近期的恶性疟原虫祖先中。我们的结果验证了用于鉴定隐秘病原体物种的选择性扩增策略,并揭示了可能使恶性疟原虫的前身易于感染人类的进化事件。

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