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全基因组测序表明,昏睡病复发是由于寄生虫再次生长,而非再次感染。

Whole genome sequencing shows sleeping sickness relapse is due to parasite regrowth and not reinfection.

作者信息

Richardson Joshua B, Evans Benjamin, Pyana Patient P, Van Reet Nick, Sistrom Mark, Büscher Philippe, Aksoy Serap, Caccone Adalgisa

机构信息

Department of Ecology and Evolutionary Biology Yale University New Haven CT USA.

Department de Parasitologie Institut National de Recherche Biomedicale Kinshasa Gombe Democratic Republic of the Congo.

出版信息

Evol Appl. 2016 Jan 9;9(2):381-93. doi: 10.1111/eva.12338. eCollection 2016 Feb.

DOI:10.1111/eva.12338
PMID:26834831
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4721075/
Abstract

The trypanosome Trypanosoma brucei gambiense (Tbg) is a cause of human African trypanosomiasis (HAT) endemic to many parts of sub-Saharan Africa. The disease is almost invariably fatal if untreated and there is no vaccine, which makes monitoring and managing drug resistance highly relevant. A recent study of HAT cases from the Democratic Republic of the Congo reported a high incidence of relapses in patients treated with melarsoprol. Of the 19 Tbg strains isolated from patients enrolled in this study, four pairs were obtained from the same patient before treatment and after relapse. We used whole genome sequencing to investigate whether these patients were infected with a new strain, or if the original strain had regrown to pathogenic levels. Clustering analysis of 5938 single nucleotide polymorphisms supports the hypothesis of regrowth of the original strain, as we found that strains isolated before and after treatment from the same patient were more similar to each other than to other isolates. We also identified 23 novel genes that could affect melarsoprol sensitivity, representing a promising new set of targets for future functional studies. This work exemplifies the utility of using evolutionary approaches to provide novel insights and tools for disease control.

摘要

布氏冈比亚锥虫(Tbg)是撒哈拉以南非洲许多地区流行的人类非洲锥虫病(HAT)的病原体。如果不进行治疗,这种疾病几乎总是致命的,而且没有疫苗,这使得监测和管理耐药性变得高度相关。最近一项对刚果民主共和国HAT病例的研究报告称,接受美拉胂醇治疗的患者复发率很高。在从参与该研究的患者中分离出的19株Tbg菌株中,有四对是从同一患者治疗前和复发后获得的。我们使用全基因组测序来研究这些患者是感染了新菌株,还是原来的菌株重新生长到了致病水平。对5938个单核苷酸多态性的聚类分析支持了原来菌株重新生长的假设,因为我们发现,从同一患者治疗前和治疗后分离出的菌株彼此之间比与其他分离株更相似。我们还鉴定出23个可能影响美拉胂醇敏感性的新基因,为未来的功能研究提供了一组有前景的新靶点。这项工作例证了使用进化方法为疾病控制提供新见解和工具的实用性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9bf0/4721075/c6a572a218f9/EVA-9-381-g002.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9bf0/4721075/c6a572a218f9/EVA-9-381-g002.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9bf0/4721075/c6a572a218f9/EVA-9-381-g002.jpg

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