Plasmodium vivax mdr1 genotypes in isolates from successfully cured patients living in endemic and non-endemic Brazilian areas

Gomes, Larissa Rodrigues; Almeida-de-Oliveira, Natália Ketrin; Lavigne, Aline Rosa de; Lima, Suelen Rezende Félix de; Pina-Costa, Anielle de; Brasil, Patrícia; Daniel-Ribeiro, Cláudio Tadeu; Ménard, Didier; Ferreira-da-Cruz, Maria de Fátima

doi:10.1186/s12936-016-1141-9

Cited by 10 publications

(17 citation statements)

References 41 publications

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“…Our study, by thoroughly characterizing these regions (that were very incompletely annotated previously), also provides an important resource to better investigate the role of these regions and their variability. One gene that would be interesting to further study based on our findings is PvMDR1, which is commonly duplicated in some endemic regions 34 and has been implicated in chloroquine or mefloquine resistance 35 , 36 . Our data clearly indicated the presence of alternatively spliced 3′-UTR introns in some transcripts, and it would be interesting to test whether these isoforms affect PvMDR1 translation or are associated with antimalarial drug resistance.…”

Section: Discussionmentioning

confidence: 90%

Characterization of P. vivax blood stage transcriptomes from field isolates reveals similarities among infections and complex gene isoforms

Kim

Popovici

Vantaux

et al. 2017

Sci Rep

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Our understanding of the structure and regulation of Plasmodium vivax genes is limited by our inability to grow the parasites in long-term in vitro cultures. Most P. vivax studies must therefore rely on patient samples, which typically display a low proportion of parasites and asynchronous parasites. Here, we present stranded RNA-seq data generated directly from a small volume of blood from three Cambodian vivax malaria patients collected before treatment. Our analyses show surprising similarities of the parasite gene expression patterns across infections, despite extensive variations in parasite stage proportion. These similarities contrast with the unique gene expression patterns observed in sporozoites isolated from salivary glands of infected Colombian mosquitoes. Our analyses also indicate that more than 10% of P. vivax genes encode multiple, often undescribed, protein-coding sequences, potentially increasing the diversity of proteins synthesized by blood stage parasites. These data also greatly improve the annotations of P. vivax gene untranslated regions, providing an important resource for future studies of specific genes.

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Section: Discussionmentioning

confidence: 90%

Characterization of P. vivax blood stage transcriptomes from field isolates reveals similarities among infections and complex gene isoforms

Kim

Popovici

Vantaux

et al. 2017

Sci Rep

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“…These temporal variations of allele frequencies could be explained by different factors, such as the increased circulation of isolates between French Guiana and Brazil or changes in drug policy for the treatment of P. falciparum . This is supported by a recent study showing that the T958M mutation allele is the majority among Brazilian isolates collected between 2010 and 2014 [42]. Many studies in Southeast Asia have shown that isolates with pvmdr1 gene amplification were characterized by increased susceptibility to chloroquine but decreased susceptibility to mefloquine [13, 31].…”

Section: Discussionmentioning

confidence: 72%

Plasmodium vivax multidrug resistance-1 gene polymorphism in French Guiana

Faway

Musset

Volney

et al. 2016

Malar J

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Background Plasmodium vivax malaria is a major public health problem in French Guiana. Some cases of resistance to chloroquine, the first-line treatment used against P. vivax malaria, have been described in the Brazilian Amazon region. The aim of this study is to investigate a possible dispersion of chloroquine-resistant P. vivax isolates in French Guiana. The genotype, polymorphism and copy number variation, of the P. vivax multidrug resistance gene-1 (pvmdr1) have been previously associated with modification of the susceptibility to chloroquine.MethodsThe pvmdr1 gene polymorphism was evaluated by sequencing and copy number variation was assessed by real-time PCR, in P. vivax isolates obtained from 591 symptomatic patients from 1997 to 2013.ResultsThe results reveal that 1.0% [95% CI 0.4–2.2] of French Guiana isolates carry the mutations Y976F and F1076L, and that the proportion of isolates with multiple copies of pvmdr1 has significantly decreased over time, from 71.3% (OR = 6.2 [95% CI 62.9–78.7], p < 0.0001) in 1997–2004 to 12.8% (OR = 0.03 [95% CI 9.4–16.9], p < 0.0001) in 2009–2013. A statistically significant relationship was found between Guf-A (harboring the single mutation T958M) and Sal-1 (wild type) alleles and pvmdr1 copy number.ConclusionsFew P. vivax isolates harboring chloroquine-resistant mutations in the pvmdr1 gene are circulating in French Guiana. However, the decrease in the prevalence of isolates carrying multiple copies of pvmdr1 might indicate that the P. vivax population in French Guiana is evolving towards a decreased susceptibility to chloroquine.

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“…Analysis of pvmdr1 sequences has shown SNPs at three codons 958, 976 and 1076 as previously described [ 6 , 12 , 15 , 17 , 19 ]. The substitution in the codon T958 M is known as an allelic variant, of which T958 wild-type was identified in Ecuador and 958M is thought being characteristic of Asia and Africa [ 12 ], while it has also been found in samples from Brazil [ 19 ]., The allelic form 958M was identified in samples from Africa and south western Asia tested here. Few isolates showed the single mutation Y976 F (4/30), in agreement with the fact that the single 976 F mutant is not very common worldwide [ 17 , 19 ].…”

Section: Discussionmentioning

confidence: 99%

“…The substitution in the codon T958 M is known as an allelic variant, of which T958 wild-type was identified in Ecuador and 958M is thought being characteristic of Asia and Africa [ 12 ], while it has also been found in samples from Brazil [ 19 ]., The allelic form 958M was identified in samples from Africa and south western Asia tested here. Few isolates showed the single mutation Y976 F (4/30), in agreement with the fact that the single 976 F mutant is not very common worldwide [ 17 , 19 ]. In contrast, many studies have reported a high prevalence of the Y976 L and/or F1076 L mutants associated with treatment failure [ 15 , 18 ].…”

Section: Discussionmentioning

confidence: 99%

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Genetic diversity of Plasmodium vivax metacaspase 1 and Plasmodium vivax multi-drug resistance 1 genes of field isolates from Mauritania, Sudan and Oman

Sow

Bonnot

Ahmed

et al. 2017

Malar J

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Background Plasmodium vivax is the second most important human malaria parasite, widely spread across the world. This parasite is associated with important issues in the process toward malaria elimination, including potential for relapse and increased resistance to chloroquine. Plasmodium vivax multi-drug resistant (pvmdr1) is suspected to be a marker of resistance although definitive evidence is lacking. Progress has been made in knowledge of biological factors affecting parasite growth, including mechanisms of regulated cell death and the suspected role of metacaspase. Plasmodium vivax metacaspase1 (PvMCA1-cd) has been described with a catalytic domain composed of histidine (H372) and cysteine (C428) residues. The aim of this study was to test for a link between the conserved histidine and cysteine residues in PvMCA1-cd, and the polymorphism of the P. vivax multi-drug resistant gene (pvmdr1).ResultsThirty P. vivax isolates were collected from Mauritania, Sudan, and Oman. Among the 28 P. vivax isolates successfully sequenced, only 4 samples showed the conserved His (372)–Cys (428) residues in PvMCA1-cd. Single nucleotide polymorphisms observed were H372T (46.4%), H372D (39.3%), and C428R (85.7%). A new polymorphic catalytic domain was observed at His (282)–Cys (305) residues. Sequences alignment analysis of pvmdr1 showed SNP in the three codons 958, 976 and 1076. A single SNP was identified at the codon M958Y (60%), 2 SNPs were found at the position 976: Y976F (13%) and Y976V (57%), and 3 SNPs were identified at the position 1076: F1076L (40%), F1076T (53%) and F1076I (3%). Only one isolate was wildtype in all three codons (MYF), 27% were single MYL mutants, and 10% were double MFL mutants. Three new haplotypes were also identified: the triple mutant YVT was most prevalent (53.3%) distributed in the three countries, while triple YFL and YVI mutants (3%), were only found in samples from Sudan and Mauritania.ConclusionsTriple or quadruple mutants for metacaspase genes and double or triple mutants for Pvmdr1 were observed in 24/28 and 19/28 samples. There was no difference in the frequency of mutations between PvMCA1-cd and Pvmdr1 (P > 0.2). Histidine and cysteine residues in PvMCA1-cd are highly polymorphic and linkage disequilibrium with SNPs of Pvmdr1 gene may be expected from these three areas with different patterns of P. vivax transmission.

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Plasmodium vivax mdr1 genotypes in isolates from successfully cured patients living in endemic and non-endemic Brazilian areas

Cited by 10 publications

References 41 publications

Characterization of P. vivax blood stage transcriptomes from field isolates reveals similarities among infections and complex gene isoforms

Characterization of P. vivax blood stage transcriptomes from field isolates reveals similarities among infections and complex gene isoforms

Plasmodium vivax multidrug resistance-1 gene polymorphism in French Guiana

Genetic diversity of Plasmodium vivax metacaspase 1 and Plasmodium vivax multi-drug resistance 1 genes of field isolates from Mauritania, Sudan and Oman

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