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恶性疟原虫的遗传多样性与氯喹选择性清除

Genetic diversity and chloroquine selective sweeps in Plasmodium falciparum.

作者信息

Wootton John C, Feng Xiaorong, Ferdig Michael T, Cooper Roland A, Mu Jianbing, Baruch Dror I, Magill Alan J, Su Xin-Zhuan

机构信息

Computational Biology Branch, National Center for Biotechnology Information, National Library of Medicine, National Institutes of Health, Bethesda, Maryland 20894-6075, USA.

出版信息

Nature. 2002 Jul 18;418(6895):320-3. doi: 10.1038/nature00813.

Abstract

Widespread use of antimalarial agents can profoundly influence the evolution of the human malaria parasite Plasmodium falciparum. Recent selective sweeps for drug-resistant genotypes may have restricted the genetic diversity of this parasite, resembling effects attributed in current debates to a historic population bottleneck. Chloroquine-resistant (CQR) parasites were initially reported about 45 years ago from two foci in southeast Asia and South America, but the number of CQR founder mutations and the impact of chlorquine on parasite genomes worldwide have been difficult to evaluate. Using 342 highly polymorphic microsatellite markers from a genetic map, here we show that the level of genetic diversity varies substantially among different regions of the parasite genome, revealing extensive linkage disequilibrium surrounding the key CQR gene pfcrt and at least four CQR founder events. This disequilibrium and its decay rate in the pfcrt-flanking region are consistent with strong directional selective sweeps occurring over only approximately 20-80 sexual generations, especially a single resistant pfcrt haplotype spreading to very high frequencies throughout most of Asia and Africa. The presence of linkage disequilibrium provides a basis for mapping genes under drug selection in P. falciparum.

摘要

抗疟药物的广泛使用会深刻影响人类疟原虫恶性疟原虫的进化。近期针对耐药基因型的选择性清除可能限制了这种寄生虫的遗传多样性,类似于当前辩论中归因于历史种群瓶颈的影响。大约45年前,在东南亚和南美洲的两个疫源地首次报告了氯喹抗性(CQR)寄生虫,但CQR起始突变的数量以及氯喹对全球寄生虫基因组的影响一直难以评估。利用遗传图谱中的342个高度多态性微卫星标记,我们在此表明,寄生虫基因组不同区域的遗传多样性水平差异很大,揭示了关键CQR基因pfcrt周围广泛的连锁不平衡以及至少四次CQR起始事件。pfcrt侧翼区域的这种不平衡及其衰减率与仅在大约20 - 80个有性世代中发生的强烈定向选择性清除一致,特别是单一抗性pfcrt单倍型在亚洲和非洲大部分地区传播到非常高的频率。连锁不平衡的存在为绘制恶性疟原虫中药物选择下的基因图谱提供了基础。

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