Plasmodium falciparum genome-wide scans for positive selection, recombination hot spots and resistance to antimalarial drugs

Mu, Jianbing; Myers, Rachel A.; Jiang, Hongying; Liu, Shengfa; Ricklefs, Stacy M.; Waisberg, Michael; Chotivanich, Kesinee; Wilairatana, Polrat; Krudsood, Srivicha; White, Nicholas J.; Udomsangpetch, Rachanee; Cui, Liwang; Ho, May; Ou, Fengzhen; Li, Haibo; Shen, Jianping; Li, Guoqiao; Wang, Xinhua; Suon, Seila; Sreng, Sokunthea; Socheat, Duong; Sturdevant, Daniel E.; Porcella, Stephen F.; Fairhurst, Rick M.; Wellems, Thomas E.; Awadalla, Philip; Su, Xin

doi:10.1038/ng.528

Cited by 182 publications

(194 citation statements)

References 32 publications

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“…Similar to previous studies of directional selection in P. falciparum, we identified drug-resistance genes (e.g., pfcrt and kelch K13) with evidence of strong directional selection (Table 3) (26)(27)(28)(29). Allele frequencies for all polymorphisms in known drugresistance genes are summarized in Table S6.…”

Section: P Vivax Shows Stronger Evidence Of Recent Directional Selecsupporting

confidence: 76%

Selective sweep suggests transcriptional regulation may underlie Plasmodium vivax resilience to malaria control measures in Cambodia

Parobek

Lin

Saunders

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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Cambodia, in which both Plasmodium vivax and Plasmodium falciparum are endemic, has been the focus of numerous malaria-control interventions, resulting in a marked decline in overall malaria incidence. Despite this decline, the number of P. vivax cases has actually increased. To understand better the factors underlying this resilience, we compared the genetic responses of the two species to recent selective pressures. We sequenced and studied the genomes of 70 P. vivax and 80 P. falciparum isolates collected between 2009 and 2013. We found that although P. falciparum has undergone population fracturing, the coendemic P. vivax population has grown undisrupted, resulting in a larger effective population size, no discernable population structure, and frequent multiclonal infections. Signatures of selection suggest recent, species-specific evolutionary differences. Particularly, in contrast to P. falciparum, P. vivax transcription factors, chromatin modifiers, and histone deacetylases have undergone strong directional selection, including a particularly strong selective sweep at an AP2 transcription factor. Together, our findings point to different population-level adaptive mechanisms used by P. vivax and P. falciparum parasites. Although population substructuring in P. falciparum has resulted in clonal outgrowths of resistant parasites, P. vivax may use a nuanced transcriptional regulatory approach to population maintenance, enabling it to preserve a larger, more diverse population better suited to facing selective threats. We conclude that transcriptional control may underlie P. vivax's resilience to malaria control measures. Novel strategies to target such processes are likely required to eradicate P. vivax and achieve malaria elimination.D uring the last decade, western Cambodia has been the focus of numerous and multimodal interventions to control the spread of artemisinin-resistant Plasmodium falciparum (1, 2). Such interventions, including increased vector control, increased surveillance, and improved access to quality artemisinin-combination therapy (ACT), would be expected to curtail coendemic Plasmodium vivax as well. However, even as P. falciparum infections in Cambodia decreased by 81% between 2009 and 2013, P. vivax cases have increased, making it the predominant species in the Mekong region (3-6). This scenario, repeated in Brazil and other areas of coendemicity, has led to growing awareness that P. vivax, although infecting the same populations and transmitted by the same mosquito vectors, will likely be the more challenging species to eradicate (6-9). In this study, we use population genomics to gain insight into the evolutionary factors underlying P. vivax's resilience to malaria control measures.Population genetic studies have previously hinted at the resilience of P. vivax populations in comparison with P. falciparum. Studies of microsatellites and highly variable antigens of sympatric P. vivax and P. falciparum populations in Southeast Asia and the Southwest Pacific have consistently shown P. viv...

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Section: P Vivax Shows Stronger Evidence Of Recent Directional Selecsupporting

confidence: 76%

Selective sweep suggests transcriptional regulation may underlie Plasmodium vivax resilience to malaria control measures in Cambodia

Parobek

Lin

Saunders

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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“…Following the generation of reference genome assemblies, malaria investigators followed the path of other organisms in the postgenomic era and characterized genomic diversity through sequencing surveys (Jeffares et al 2007;Mu et al 2007;Volkman et al 2007;Tan et al 2011;Neafsey et al 2012) and later genome-wide single nucleotide polymorphism (SNP) arrays (Neafsey et al , 2010Mu et al 2010;Tan et al 2011;Van Tyne et al 2011). Such work illuminated the recent demographic history of multiple parasite and vector species, defined sometimes complex gene flow boundaries, and revealed the impact of immune, drug, or insecticide selection on the genomes of malaria parasites and vectors.…”

Section: An Abundance Of Genomic Datamentioning

confidence: 99%

Malaria Genomics in the Era of Eradication

Neafsey

Volkman

2017

Cold Spring Harb Perspect Med

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The first reference genome assembly for the Plasmodium falciparum malaria parasite was completed over a decade ago, and the impact of this and other genomic resources on malaria research has been significant. Genomic resources for other malaria parasites are being established, even as P. falciparum continues to be the focus of development of new genomic methods and applications. Here we review the impact and applications of genomic data on malaria research, and discuss future needs and directions as genomic data generation becomes less expensive and more decentralized. Specifically, we focus on how population genomic strategies can be utilized to advance the malaria eradication agenda.

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“…Once prepared, these libraries can be examined in a host of biological processes, here exemplified with a neglected disease of the third world for discovery of probes and future drugs. In our collaborative effort, the CMLD-BU compound collection was assayed for antimalarial activity against five lines of P. falciparum with distinct geographic origins, representing genotypic variation in part resulting from acquired antimalarial drug resistance (16). Overall, the CMLD-BU compound collection provided an effective source of chemotypes in the antimalaria assays.…”

Section: Resultsmentioning

confidence: 99%

“…Detailed procedures for the synthesis of indoline alkadoids are outlined in previous publications (14,16). Characterization of biologically active indoline alkaloids are provided in the SI Appendix.…”

Section: Methodsmentioning

confidence: 99%

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Discovery of new antimalarial chemotypes through chemical methodology and library development

Brown

Cheng

Wei

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

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In an effort to expand the stereochemical and structural complexity of chemical libraries used in drug discovery, the Center for Chemical Methodology and Library Development at Boston University has established an infrastructure to translate methodologies accessing diverse chemotypes into arrayed libraries for biological evaluation. In a collaborative effort, the NIH Chemical Genomics Center determined IC 50 's for Plasmodium falciparum viability for each of 2,070 members of the CMLD-BU compound collection using quantitative high-throughput screening across five parasite lines of distinct geographic origin. Three compound classes displaying either differential or comprehensive antimalarial activity across the lines were identified, and the nascent structure activity relationships (SAR) from this experiment used to initiate optimization of these chemotypes for further development.T he synthesis of compound libraries embodying structural diversity and complexity is one potential avenue to enabling the discovery of potent and selective bioactive agents (1-3). Synthetic methodology aimed at library design and distribution is the focus of the Center for Chemical Methodology and Library Development at Boston University (CMLD-BU). Currently the CMLD-BU maintains a collection of approximately 2,500 compounds derived from reaction methodologies developed in the Center and associated groups. The CMLD-BU has developed a workflow that leverages focused methodology development (4) and identification of new scaffolds and chemical reactions utilizing multidimensional reaction screening (5) for the synthesis of libraries.In a collaboration between the CMLD-BU and the NIH Chemical Genomics Center (NCGC), an effort to discover unique chemotypes which inhibit the viability of P. falciparum, the causative agent of malaria, is underway. Malaria not only inflicts tremendous suffering and morbidity on the human population, but has dramatically influenced the course of civilization with profound sociological and economic implications (6). In response, there have been significant screening efforts for new antimalarial agents (7,8). Effective treatments continue to be needed in part due to acquired resistance of P. falciparum. Identification of molecular targets affecting the viability of malaria is necessary for efficient drug development as is the discovery of chemotypes active across a variety of geographic isolates. With an aim to improve the process of identifying new compounds and targets, we have used quantitative high-throughput screening (qHTS) to achieve pharmacological fingerprints of chemical libraries (9). This technique tests each compound as a seven point titration covering four orders of magnitude in concentration thus allowing sufficient resolving power by virtue of IC 50 determinations to reveal subtle differences in compound activities between parasite lines. A compound with a differential chemical phenotype (DCP) can enable mapping of target genes using genetic recombination wherein the DCP emerges between two or more...

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Plasmodium falciparum genome-wide scans for positive selection, recombination hot spots and resistance to antimalarial drugs

Cited by 182 publications

References 32 publications

Selective sweep suggests transcriptional regulation may underlie Plasmodium vivax resilience to malaria control measures in Cambodia

Selective sweep suggests transcriptional regulation may underlie Plasmodium vivax resilience to malaria control measures in Cambodia

Malaria Genomics in the Era of Eradication

Discovery of new antimalarial chemotypes through chemical methodology and library development

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