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利用同源性量化本地恶性疟原虫种群之间的连通性。

Quantifying connectivity between local Plasmodium falciparum malaria parasite populations using identity by descent.

作者信息

Taylor Aimee R, Schaffner Stephen F, Cerqueira Gustavo C, Nkhoma Standwell C, Anderson Timothy J C, Sriprawat Kanlaya, Pyae Phyo Aung, Nosten François, Neafsey Daniel E, Buckee Caroline O

机构信息

Center for Communicable Disease Dynamics, Department of Epidemiology, Harvard T.H. Chan School of Public Health, Boston, Massachusetts, United States of America.

Infectious Disease and Microbiome Program, Broad Institute, Cambridge, Massachusetts, United States of America.

出版信息

PLoS Genet. 2017 Oct 27;13(10):e1007065. doi: 10.1371/journal.pgen.1007065. eCollection 2017 Oct.

Abstract

With the rapidly increasing abundance and accessibility of genomic data, there is a growing interest in using population genetic approaches to characterize fine-scale dispersal of organisms, providing insight into biological processes across a broad range of fields including ecology, evolution and epidemiology. For sexually recombining haploid organisms such as the human malaria parasite P. falciparum, however, there have been no systematic assessments of the type of data and methods required to resolve fine scale connectivity. This analytical gap hinders the use of genomics for understanding local transmission patterns, a crucial goal for policy makers charged with eliminating this important human pathogen. Here we use data collected from four clinics with a catchment area spanning approximately 120 km of the Thai-Myanmar border to compare the ability of divergence (FST) and relatedness based on identity by descent (IBD) to resolve spatial connectivity between malaria parasites collected from proximal clinics. We found no relationship between inter-clinic distance and FST, likely due to sampling of highly related parasites within clinics, but a significant decline in IBD-based relatedness with increasing inter-clinic distance. This association was contingent upon the data set type and size. We estimated that approximately 147 single-infection whole genome sequenced parasite samples or 222 single-infection parasite samples genotyped at 93 single nucleotide polymorphisms (SNPs) were sufficient to recover a robust spatial trend estimate at this scale. In summary, surveillance efforts cannot rely on classical measures of genetic divergence to measure P. falciparum transmission on a local scale. Given adequate sampling, IBD-based relatedness provides a useful alternative, and robust trends can be obtained from parasite samples genotyped at approximately 100 SNPs.

摘要

随着基因组数据的丰富程度和可获取性迅速增加,人们越来越有兴趣使用群体遗传学方法来描述生物体的精细尺度扩散,从而深入了解包括生态学、进化和流行病学在内的广泛领域中的生物过程。然而,对于像人类疟原虫恶性疟原虫这样进行有性重组的单倍体生物,尚未对解析精细尺度连通性所需的数据类型和方法进行系统评估。这一分析空白阻碍了利用基因组学来理解局部传播模式,而这是负责消除这种重要人类病原体的政策制定者的关键目标。在此,我们使用从泰国 - 缅甸边境约120公里集水区内的四家诊所收集的数据,比较基于分化(FST)和基于血缘同一性(IBD)的亲缘关系来解析从相邻诊所收集的疟原虫之间空间连通性的能力。我们发现诊所间距离与FST之间没有关系,这可能是由于诊所内采样的是高度相关的寄生虫,但基于IBD的亲缘关系随着诊所间距离增加而显著下降。这种关联取决于数据集的类型和大小。我们估计,大约147个单感染全基因组测序的寄生虫样本或222个在93个单核苷酸多态性(SNP)处进行基因分型的单感染寄生虫样本足以在这个尺度上恢复稳健的空间趋势估计。总之,监测工作不能依赖传统的遗传分化测量方法来在局部尺度上衡量恶性疟原虫的传播。在有足够采样的情况下,基于IBD的亲缘关系提供了一个有用的替代方法,并且从大约100个SNP进行基因分型的寄生虫样本中可以获得稳健的趋势。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/92aa/5678785/53f82ea3f50d/pgen.1007065.g001.jpg

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