Title
Molecular surveillance of the Plasmodium vivax multidrug resistance 1 gene in Peru between 2006 and 2015
Date Issued
01 December 2020
Access level
open access
Resource Type
journal article
Author(s)
U.S. Naval Medical Research Unit No 6
U.S. Naval Medical Research Unit No 6
U.S. Naval Medical Research Unit No 6
Publisher(s)
BioMed Central Ltd
Abstract
Background: The high incidence of Plasmodium vivax infections associated with clinical severity and the emergence of chloroquine (CQ) resistance has posed a challenge to control efforts aimed at eliminating this disease. Despite conflicting evidence regarding the role of mutations of P. vivax multidrug resistance 1 gene (pvmdr1) in drug resistance, this gene can be a tool for molecular surveillance due to its variability and spatial patterns. Methods: Blood samples were collected from studies conducted between 2006 and 2015 in the Northern and Southern Amazon Basin and the North Coast of Peru. Thick and thin blood smears were prepared for malaria diagnosis by microscopy and PCR was performed for detection of P. vivax monoinfections. The pvmdr1 gene was subsequently sequenced and the genetic data was used for haplotype and diversity analysis. Results: A total of 550 positive P. vivax samples were sequenced; 445 from the Northern Amazon Basin, 48 from the Southern Amazon Basin and 57 from the North Coast. Eight non-synonymous mutations and three synonymous mutations were analysed in 4,395 bp of pvmdr1. Amino acid changes at positions 976F and 1076L were detected in the Northern Amazon Basin (12.8%) and the Southern Amazon Basin (4.2%) with fluctuations in the prevalence of both mutations in the Northern Amazon Basin during the course of the study that seemed to correspond with a malaria control programme implemented in the region. A total of 13 pvmdr1 haplotypes with non-synonymous mutations were estimated in Peru and an overall nucleotide diversity of π = 0.00054. The Northern Amazon Basin was the most diverse region (π = 0.00055) followed by the Southern Amazon and the North Coast (π = 0.00035 and π = 0.00014, respectively). Conclusion: This study showed a high variability in the frequencies of the 976F and 1076L polymorphisms in the Northern Amazon Basin between 2006 and 2015. The low and heterogeneous diversity of pvmdr1 found in this study underscores the need for additional research that can elucidate the role of this gene on P. vivax drug resistance as well as in vitro and clinical data that can clarify the extend of CQ resistance in Peru.
Volume
19
Issue
1
Language
English
OCDE Knowledge area
Parasitología
Subjects
Scopus EID
2-s2.0-85097077537
PubMed ID
Source
Malaria Journal
ISSN of the container
1475-2875
Source project
Sponsor(s)
We thank to Dionicia Gamboa, PhD and Joseph Vinetz, MD and the investigators, field team members and study participants from the Amazonia Center of Excellence in Malaria Research, funded by cooperative agreement U19AI089681 from the United States Public Health Service, NIH/NIAID.
We would like to express our gratitude to ?Direcci?n Regional de Salud Piura? for the logistic support and in executing the blood samples collection for the ?NMRCD.2010.0010? protocol. AGL is sponsored by the training grant D43 TW007393 awarded by the Fogarty International Center of the US National Institutes of Health awarded to Emerge, the Emerging Diseases and Climate Change Research Unit of the School and Public Health Administration at Universidad Peruana Cayetano Heredia. Meddly Santolalla received a scholarship from CAPES ? Coordination for the Improvement of Higher Education Personnel. Jorge L. Magui?a is a doctoral student studying Epidemiological Research at Universidad Peruana Cayetano Heredia under FONDECYT/CIENCIACTIVA scholarship EF033-235-2015 and supported by training grant D43 TW007393 awarded by the Fogarty International Center of the US National Institutes of Health. We thank to Dionicia Gamboa, PhD and Joseph Vinetz, MD and the investigators, field team members and study participants from the Amazonia Center of Excellence in Malaria Research, funded by cooperative agreement U19AI089681 from the United States Public Health Service, NIH/NIAID.
AGL is sponsored by the training grant D43 TW007393 awarded by the Fogarty International Center of the US National Institutes of Health awarded to Emerge, the Emerging Diseases and Climate Change Research Unit of the School and Public Health Administration at Universidad Peruana Cayetano Heredia. Meddly Santolalla received a scholarship from CAPES – Coordination for the Improvement of Higher Education Personnel. Jorge L. Maguiña is a doctoral student studying Epidemiological Research at Universidad Peruana Cayetano Heredia under FONDECYT/CIENCIACTIVA scholarship EF033-235-2015 and supported by training grant D43 TW007393 awarded by the Fogarty International Center of the US National Institutes of Health.
This study was supported by funding from the US Department of Defense Health Agency-Armed Forces Health Surveillance Division (AFHSD), Global Emerging Infection Surveillance (GEIS) under PROMIS ID P0106_18_N6_02.
Sources of information:
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