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猴子的故事:间日疟原虫作为人类疟原虫的起源

A monkey's tale: the origin of Plasmodium vivax as a human malaria parasite.

作者信息

Escalante Ananias A, Cornejo Omar E, Freeland Denise E, Poe Amanda C, Durrego Ester, Collins William E, Lal Altaf A

机构信息

Division of Parasitic Diseases, Centers for Disease Control and Prevention, Chamblee, GA 30341, USA.

出版信息

Proc Natl Acad Sci U S A. 2005 Feb 8;102(6):1980-5. doi: 10.1073/pnas.0409652102. Epub 2005 Jan 31.

Abstract

The high prevalence of Duffy negativity (lack of the Duffy blood group antigen) among human populations in sub-Saharan Africa has been used to argue that Plasmodium vivax originated on that continent. Here, we investigate the phylogenetic relationships among 10 species of Plasmodium that infect primates by using three genes, two nuclear (beta-tubulin and cell division cycle 2) and a gene from the plastid genome (the elongation factor Tu). We find compelling evidence that P. vivax is derived from a species that inhabited macaques in Southeast Asia. Specifically, those phylogenies that include P. vivax as an ancient lineage from which all of the macaque parasites could originate are significantly less likely to explain the data. We estimate the time to the most recent common ancestor at four neutral gene loci from Asian and South American isolates (a minimum sample of seven isolates per locus). Our analysis estimates that the extant populations of P. vivax originated between 45,680 and 81,607 years ago. The phylogeny and the estimated time frame for the origination of current P. vivax populations are consistent with an "out of Asia" origin for P. vivax as hominoid parasite. The current debate regarding how the Duffy negative trait became fixed in Africa needs to be revisited, taking into account not only human genetic data but also the genetic diversity observed in the extant P. vivax populations and the phylogeny of the genus Plasmodium.

摘要

在撒哈拉以南非洲人群中,达菲阴性(缺乏达菲血型抗原)的高流行率被用来支持间日疟原虫起源于该大陆的观点。在此,我们通过使用三个基因(两个核基因,即β - 微管蛋白和细胞分裂周期蛋白2,以及一个来自质体基因组的基因,即延伸因子Tu)来研究感染灵长类动物的10种疟原虫之间的系统发育关系。我们发现了令人信服的证据,表明间日疟原虫源自一种栖息于东南亚猕猴体内的物种。具体而言,那些将间日疟原虫作为所有猕猴寄生虫可能起源的古老谱系的系统发育树,解释这些数据的可能性要小得多。我们从亚洲和南美分离株的四个中性基因位点估计了最近共同祖先的时间(每个位点至少有七个分离株的样本)。我们的分析估计,现存的间日疟原虫种群起源于45680至81607年前。间日疟原虫当前种群起源的系统发育和估计时间框架与作为类人猿寄生虫的间日疟原虫“走出亚洲”的起源一致。关于达菲阴性性状如何在非洲固定下来的当前争论需要重新审视,不仅要考虑人类遗传数据,还要考虑现存间日疟原虫种群中观察到的遗传多样性以及疟原虫属的系统发育。

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