Recurrent Parasitemias and Population Dynamics of Plasmodium vivax Polymorphisms in Rural Amazonia

Orjuela-Sánchez, Pamela; Silva, Natal Santos da; Silva‐Nunes, Mônica da; Ferreira, Marcelo U.

doi:10.4269/ajtmh.2009.09-0337

Cited by 76 publications

(104 citation statements)

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“…Parasites were systematically sampled over 30 months (April 2004 through October 2006) in one of the study sites in Brazil, Granada [11,16]. We hypothesized that local parasite populations gradually diversify over time as a result of migration, genetic drift, mutation and recombination.…”

Section: Resultsmentioning

confidence: 99%

“…The 249 samples from Brazil were collected in the rural settlement of Granada and the town of Plácido de Castro (50 km south of Granada), both in Acre State, and in the city of Porto Velho (500 km east of Granada), in Rondônia State. The samples from Granada (n = 193) were collected during prospective cohort studies between 2004 and 2006 [11,16,30], those from Plácido de Castro (n = 38) were collected in 2008 from patients attending the town's malaria clinic [31], and those from Porto Velho (n = 17) were collected from patients attending the Oswaldo Cruz Outpatient Clinic in June-July 1995 [32]. The 70 samples from Cambodia were collected between June and December 2008 in Pursat town from individuals who became infected in the nearby forests (ClinicalTrials.gov identifier, NCT00663546).…”

Section: Methodsmentioning

confidence: 99%

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Single-nucleotide polymorphism, linkage disequilibrium and geographic structure in the malaria parasite Plasmodium vivax: prospects for genome-wide association studies

et al. 2010

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BackgroundThe ideal malaria parasite populations for initial mapping of genomic regions contributing to phenotypes such as drug resistance and virulence, through genome-wide association studies, are those with high genetic diversity, allowing for numerous informative markers, and rare meiotic recombination, allowing for strong linkage disequilibrium (LD) between markers and phenotype-determining loci. However, levels of genetic diversity and LD in field populations of the major human malaria parasite P. vivax remain little characterized.ResultsWe examined single-nucleotide polymorphisms (SNPs) and LD patterns across a 100-kb chromosome segment of P. vivax in 238 field isolates from areas of low to moderate malaria endemicity in South America and Asia, where LD tends to be more extensive than in holoendemic populations, and in two monkey-adapted strains (Salvador-I, from El Salvador, and Belem, from Brazil). We found varying levels of SNP diversity and LD across populations, with the highest diversity and strongest LD in the area of lowest malaria transmission. We found several clusters of contiguous markers with rare meiotic recombination and characterized a relatively conserved haplotype structure among populations, suggesting the existence of recombination hotspots in the genome region analyzed. Both silent and nonsynonymous SNPs revealed substantial between-population differentiation, which accounted for ~40% of the overall genetic diversity observed. Although parasites clustered according to their continental origin, we found evidence for substructure within the Brazilian population of P. vivax. We also explored between-population differentiation patterns revealed by loci putatively affected by natural selection and found marked geographic variation in frequencies of nucleotide substitutions at the pvmdr-1 locus, putatively associated with drug resistance.ConclusionThese findings support the feasibility of genome-wide association studies in carefully selected populations of P. vivax, using relatively low densities of markers, but underscore the risk of false positives caused by population structure at both local and regional levels.See commentary: http://www.biomedcentral.com/1741-7007/8/90

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Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Single-nucleotide polymorphism, linkage disequilibrium and geographic structure in the malaria parasite Plasmodium vivax: prospects for genome-wide association studies

et al. 2010

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“…33 We have shown that by adding more polymorphic markers into the analysis, the proportion if identical genotypes may be even lower than what we found with msp3-alpha. For example, a similar study in Brazil 34 has found very few 14-marker haplotypes in recurrent P. vivax infections using microsatellite typing. In this study, we considered a 5% tolerance in band sizes for TR markers to consider the possibility that relapsing parasites may be a minor, genetically different parasite clone that could have missed when typing parasites at the reference infection.…”

Section: Discussionmentioning

confidence: 99%

Microgeographical Differences of Plasmodium vivax Relapse and Re-Infection in the Peruvian Amazon

Chuquiyauri

Peñataro

Brouwer

et al. 2013

The American Journal of Tropical Medicine and Hygiene

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Abstract. To determine the magnitude of Plasmodium vivax relapsing malaria in rural Amazonia, we carried out a study in four sites in northeastern Peru. Polymerase chain reaction-restriction fragment length polymorphism of PvMSP3a and tandem repeat (TR) markers were compared for their ability to distinguish relapse versus reinfection. Of 1,507 subjects with P. vivax malaria, 354 developed 1 episode during the study; 97 of 354 (27.5%) were defined as relapse using Pvmsp-3a alone. The addition of TR polymorphism analysis significantly reduced the number of definitively defined relapses to 26 of 354 (7.4%) (P 0.05). Multivariate logistic regression modeling showed that the probability of having 1 infection was associated with the following: subjects in Mazan (odds ratio [OR] = 2.56; 95% confidence interval [CI] 1.87, 3.51), 15-44 years of age (OR = 1.49; 95% CI 1.03, 2.15), traveling for job purposes (OR = 1.45; 95%CI 1.03, 2.06), and travel within past month (OR = 1.46; 95% CI 1.0, 2.14). The high discriminatory capacity of the molecular tools shown here is useful for understanding the micro-geography of malaria transmission.

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“…In contrast to the ~1,000 polymorphic microsatellite loci currently available for P. falciparum typing, it was demonstrated that a few dozen microsatellite loci are polymorphic in P. vivax field isolates (Table II). Despite these limitations, microsatellite-based studies of the parasite have provided valuable information on P. vivax population structure and diversity in the Americas, Asia and Africa (Ferreira et al 2007, Karunaweera et al 2007, Koepfli et al 2009, Orjuela-Sánchez et al 2009a, Gunawardena et al 2010, Rezende et al 2010, Van den Eede et al 2010a, b, 2011). …”

Section: Neutral or Nearly Neutral Molecular Markersmentioning

confidence: 99%

“…For example, in 90 P. vivax isolates from Thailand, Cui et al (2003b) found a multiple-clone infection rate of 25.6% using the PvCSP encoding gene alone, 19.3% using PvMSP-3α alone and 35.6% when the markers were combined. Particularly surprising is the extensive clonal diversity of P. vivax infections in areas with relatively low malaria transmission, such as Brazil, Colombia and Sri Lanka (Ferreira et al 2007, Imwong et al 2007b, Karunaweera et al 2008, Orjuela-Sánchez et al 2009a, Gunawardena et al 2010. The evolutionary and epidemiological consequences of multiple-clone P. vivax infections have not been well-investigated.…”

Section: Neutral or Nearly Neutral Molecular Markersmentioning

confidence: 99%

Molecular markers and genetic diversity of Plasmodium vivax

Brito

Ferreira

2011

Mem. Inst. Oswaldo Cruz

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Enhanced understanding of the transmission dynamics and population genetics for Key words: malaria -Plasmodium vivax -genetic markers -genetic diversity -multiple-clone infections -microsatellitesMarkers and genetic diversity of P. vivax • Cristiana Ferreira Alves de Brito, Marcelo Urbano Ferreira 13 tual heterozygosity (H E ) values. Virtual H E is the average probability that a pair of alleles randomly obtained from the population is different. Whenever appropriate, in this review we provide H E estimates obtained using different markers for different populations.Molecular markers under selection -Until recently, most genetic markers available for characterising natural P. vivax populations were orthologues of previously identified P. falciparum antigen-coding genes. The wellcharacterised polymorphic regions in these genes have been extensively used to analyse genetic diversity patterns in P. falciparum (Roy et al. 2008). A similar approach has been explored in vivax-oriented studies (Cui et al. 2003a). The following single-copy genes in P. vivax have often been used in these studies: gam1, coding for the gametocyte antigen 1, csp, coding for the circumsporozoite protein (CSP), msp1 and msp3alpha, coding for the merozoite surface proteins (MSP)-1 and 3α, respectively, ama1, coding for the apical membrane antigen 1, and dbp, coding for the Duffy binding protein (DBP) ( Table I).A notable feature of several P. vivax surface antigens (including major vaccine-candidate molecules) is tandem arrays of relatively short amino acid motifs. The CSP in P. vivax (PvCSP), an abundant antigen on the surface of sporozoites that has been extensively used as a vaccine development target, has immunodominant B-cell epitopes that map to central repeats between nonrepetitive sequences (Nardin & Zavala 1998). PvCSP displays two major types of nonapeptide repeats [most commonly GDRA(D/A)GQPA and ANGA(G/D)(N/D)QPG], which define the variants known as VK210 and VK247, respectively (Arnot et al. 1985, Rosenberg et al. 1989 (Fig. 1). Both VK210 and VK247 variants are globally distributed, but geographic biases have been described (Cochrane et al. 1990, Qari et al. 1993a. Similar repetitive sequences are found in Brazil, Southeast Asia and Papua New Guinea (Qari et al. 1991(Qari et al. , 1992. However, markedly divergent sequence variants were found in isolates from China and North Korea (Mann et al. 1994). Although VK210 and VK247-type sequences often occur in sympatric parasite populations, there are no examples of a hybrid repeat array with both repeat types (Lim et al. 2005).A third type of repeat unit [APGANQ(E/G)GAA], identical to that described for Plasmodium simiovale, characterises the so-called P. vivax-like parasites (Qari et al. 1993a). Although P. vivax-like CSP repeats have been found in parasite isolates across the world, its global distribution remains unconfirmed (Gopinath et al. 1994). In Brazil, P. vivax-like parasites have been identified only in mixed-clone infections with VK210-type or VK247-type parasites (Machado...

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Recurrent Parasitemias and Population Dynamics of Plasmodium vivax Polymorphisms in Rural Amazonia

Cited by 76 publications

References 38 publications

Single-nucleotide polymorphism, linkage disequilibrium and geographic structure in the malaria parasite Plasmodium vivax: prospects for genome-wide association studies

Single-nucleotide polymorphism, linkage disequilibrium and geographic structure in the malaria parasite Plasmodium vivax: prospects for genome-wide association studies

Microgeographical Differences of Plasmodium vivax Relapse and Re-Infection in the Peruvian Amazon

Molecular markers and genetic diversity of Plasmodium vivax

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