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9 results on '"Fredy E. Villena"'

1. Drug resistance and population structure of Plasmodium falciparum and Plasmodium vivax in the Peruvian Amazon

Author

Fredy E. Villena, Juan F. Sanchez, Oscar Nolasco, Greys Braga, Leonila Ricopa, Keare Barazorda, Carola J. Salas, Carmen Lucas, Stephen E. Lizewski, Christie A. Joya, Dionicia Gamboa, Christopher Delgado-Ratto, and Hugo O. Valdivia

Subjects
Medicine, Science
Abstract

Abstract Malaria is a major health problem in Peru despite substantial progress achieved by the ongoing malaria elimination program. This study explored the population genetics of 63 Plasmodium falciparum and 170 P. vivax cases collected in the Peruvian Amazon Basin between 2015 and 2019. Microscopy and PCR were used for malaria detection and positive samples were genotyped at neutral and drug resistance-associated regions. The P. falciparum population exhibited a low nucleotide diversity (π = 0.02) whereas the P. vivax population presented a higher genetic diversity (π = 0.34). All P. falciparum samples (n = 63) carried chloroquine (CQ) resistant mutations on Pfcrt. Most P. falciparum samples (53 out of 54) carried sulfadoxine (SD) resistant mutations on Pfdhfr and Pfdhps. No evidence was found of artemisinin resistance mutations on kelch13. Population structure showed that a single cluster accounted for 93.4% of the P. falciparum samples whereas three clusters were found for P. vivax. Our study shows a low genetic diversity for both species with significant differences in genetic sub-structuring. The high prevalence of CQ-resistance mutations could be a result of indirect selection pressures driven by the P. vivax treatment scheme. These results could be useful for public health authorities to safeguard the progress that Peru has achieved towards malaria elimination.

Published
2022
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2. Population genomics and evidence of clonal replacement of Plasmodium falciparum in the Peruvian Amazon

Author

Fredy E. Villena, Stephen E. Lizewski, Christie A. Joya, and Hugo O. Valdivia

Subjects
Medicine, Science
Abstract

Abstract Previous studies have shown that P. falciparum parasites in South America have undergone population bottlenecks resulting in clonal lineages that are differentially distributed and that have been responsible for several outbreaks different endemic regions. In this study, we explored the genomic profile of 18 P. falciparum samples collected in the Peruvian Amazon Basin (Loreto) and 6 from the Peruvian North Coast (Tumbes). Our results showed the presence of three subpopulations that matched previously typed lineages in Peru: Bv1 (n = 17), Clonet D (n = 4) and Acre-Loreto type (n = 3). Gene coverage analysis showed that none of the Bv1 samples presented coverage for pfhrp2 and pfhrp3. Genotyping of drug resistance markers showed a high prevalence of Chloroquine resistance mutations S1034C/N1042D/D1246Y in pfmdr1 (62.5%) and K45T in pfcrt (87.5%). Mutations associated with sulfadoxine and pyrimethamine treatment failure were found on 88.8% of the Bv1 samples which were triple mutants for pfdhfr (50R/51I/108N) and pfdhps (437G/540E/581G). Analysis of the pfS47 gene that allows P. falciparum to evade mosquito immune responses showed that the Bv1 lineage presented one pfS47 haplotype exclusive to Loreto and another haplotype that was present in both Loreto and Tumbes. Furthermore, a possible expansion of Bv1 was detected since 2011 in Loreto. This replacement could be a result of the high prevalence of CQ resistance polymorphisms in Bv1, which could have provided a selective advantage to the indirect selection pressures driven by the use of CQ for P. vivax treatment.

Published
2021
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3. Molecular surveillance of the Plasmodium vivax multidrug resistance 1 gene in Peru between 2006 and 2015

Author

Fredy E. Villena, Jorge L. Maguiña, Meddly L. Santolalla, Edwar Pozo, Carola J. Salas, Julia S. Ampuero, Andres G. Lescano, Danett K. Bishop, and Hugo O. Valdivia

Subjects
Malaria, Plasmodium vivax, Single nucleotide polymorphisms, Drug resistance, Arctic medicine. Tropical medicine, RC955-962, Infectious and parasitic diseases, RC109-216
Abstract

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.

Published
2020
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4. Population genomics and evidence of clonal replacement of Plasmodium falciparum in the Peruvian Amazon

Author

Hugo O. Valdivia, Fredy E. Villena, Christie A. Joya, and Stephen E. Lizewski

Subjects
Lineage (genetic), Sulfadoxine, medicine.medical_treatment, Science, Plasmodium falciparum, Antiprotozoal Agents, Drug Resistance, Drug resistance, Mosquito Vectors, Polymorphism, Single Nucleotide, Article, Population genomics, Evolution, Molecular, Gene Frequency, Peru, parasitic diseases, medicine, Genotyping, Genetics, Multidisciplinary, biology, Haplotype, Parasite genomics, Outbreak, Chloroquine, Genomics, biology.organism_classification, Pyrimethamine, Medicine, Genome, Protozoan
Abstract

Previous studies have shown that P. falciparum parasites in South America have undergone population bottlenecks resulting in clonal lineages that are differentially distributed and that have been responsible for several outbreaks different endemic regions. In this study, we explored the genomic profile of 18 P. falciparum samples collected in the Peruvian Amazon Basin (Loreto) and 6 from the Peruvian North Coast (Tumbes). Our results showed the presence of three subpopulations that matched previously typed lineages in Peru: Bv1 (n = 17), Clonet D (n = 4) and Acre-Loreto type (n = 3). Gene coverage analysis showed that none of the Bv1 samples presented coverage for pfhrp2 and pfhrp3. Genotyping of drug resistance markers showed a high prevalence of Chloroquine resistance mutations S1034C/N1042D/D1246Y in pfmdr1 (62.5%) and K45T in pfcrt (87.5%). Mutations associated with sulfadoxine and pyrimethamine treatment failure were found on 88.8% of the Bv1 samples which were triple mutants for pfdhfr (50R/51I/108N) and pfdhps (437G/540E/581G). Analysis of the pfS47 gene that allows P. falciparum to evade mosquito immune responses showed that the Bv1 lineage presented one pfS47 haplotype exclusive to Loreto and another haplotype that was present in both Loreto and Tumbes. Furthermore, a possible expansion of Bv1 was detected since 2011 in Loreto. This replacement could be a result of the high prevalence of CQ resistance polymorphisms in Bv1, which could have provided a selective advantage to the indirect selection pressures driven by the use of CQ for P. vivax treatment.

Published
2021

6. Molecular surveillance of the Plasmodium vivax multidrug resistance 1 gene in Peru between 2006 and 2015

Author

Danett K. Bishop, Fredy E. Villena, Andres G. Lescano, Hugo O. Valdivia, Jorge L. Maguiña, Meddly L. Santolalla, Carola J. Salas, Edwar Pozo, and Julia S. Ampuero

Subjects
0301 basic medicine, lcsh:Arctic medicine. Tropical medicine, lcsh:RC955-962, purl.org/pe-repo/ocde/ford#3.03.07 [https], 030231 tropical medicine, Plasmodium vivax, Protozoan Proteins, Zoology, Drug resistance, purl.org/pe-repo/ocde/ford#3.03.08 [https], Biology, Polymorphism, Single Nucleotide, Nucleotide diversity, lcsh:Infectious and parasitic diseases, Insecticide Resistance, 03 medical and health sciences, Antimalarials, 0302 clinical medicine, parasitic diseases, medicine, Malaria, Vivax, Prevalence, Humans, lcsh:RC109-216, purl.org/pe-repo/ocde/ford#1.03.01 [http], Molecular Epidemiology, Amazon rainforest, Research, Haplotype, Single nucleotide polymorphisms, biology.organism_classification, medicine.disease, Malaria, 030104 developmental biology, Infectious Diseases, Cross-Sectional Studies, Parasitology, Multidrug Resistance-Associated Proteins, Synonymous substitution, geographic locations
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.

Published
2020

7. The Amazonian Tropical Bites Research Initiative, a hope for resolving zoonotic neglected tropical diseases in the One Health era

Author

Emma Taylor, Elsa Gladys Aguilar-Ancori, Ashley C Banyard, Isis Abel, Clara Mantini-Briggs, Charles L Briggs, Carolina Carrillo, Cesar M Gavidia, Ricardo Castillo-Neyra, Alejandro D Parola, Fredy E Villena, Joaquin M Prada, Brett W Petersen, Nestor Falcon Perez, Cesar Cabezas Sanchez, Moises Sihuincha, Daniel G Streicker, Ciro Maguina Vargas, Ana Maria Navarro Vela, Marco A N Vigilato, Hui Wen Fan, Rodney Willoughby, Daniel L Horton, and Sergio E Recuenco

Subjects
Health (social science), indigenous populations, bites, Public Health, Environmental and Occupational Health, General Medicine, infectious diseases, Amazon, neglected disease, zoonoses
Abstract

Background Neglected tropical diseases (NTDs) disproportionately affect populations living in resource-limited settings. In the Amazon basin, substantial numbers of NTDs are zoonotic, transmitted by vertebrate (dogs, bats, snakes) and invertebrate species (sand flies and triatomine insects). However, no dedicated consortia exist to find commonalities in the risk factors for or mitigations against bite-associated NTDs such as rabies, snake envenoming, Chagas disease and leishmaniasis in the region. The rapid expansion of COVID-19 has further reduced resources for NTDs, exacerbated health inequality and reiterated the need to raise awareness of NTDs related to bites. Methods The nine countries that make up the Amazon basin have been considered (Bolivia, Brazil, Colombia, Ecuador, French Guiana, Guyana, Peru, Surinam and Venezuela) in the formation of a new network. Results The Amazonian Tropical Bites Research Initiative (ATBRI) has been created, with the aim of creating transdisciplinary solutions to the problem of animal bites leading to disease in Amazonian communities. The ATBRI seeks to unify the currently disjointed approach to the control of bite-related neglected zoonoses across Latin America. Conclusions The coordination of different sectors and inclusion of all stakeholders will advance this field and generate evidence for policy-making, promoting governance and linkage across a One Health arena.

Published
2021

8. Genomic surveillance of Plasmodium falciparum and Plasmodium vivax cases at the University Hospital in Tegucigalpa, Honduras

Author

Hugo O. Valdivia, Fredy E. Villena, Jackeline Alger, Danett K. Bishop, Jorge García, and Stephen E. Lizewski

Subjects
0301 basic medicine, 030231 tropical medicine, Plasmodium vivax, Plasmodium falciparum, Drug Resistance, Drug resistance, Biology, Polymorphism, Single Nucleotide, Article, Specimen Handling, Hospitals, University, 03 medical and health sciences, 0302 clinical medicine, Chloroquine, parasitic diseases, medicine, Malaria, Vivax, Parasite hosting, Cluster Analysis, Humans, Malaria, Falciparum, Genotyping, Phylogeny, Likelihood Functions, Multidisciplinary, Genome, Haplotype, Biodiversity, Genomics, medicine.disease, biology.organism_classification, Virology, Malaria, 030104 developmental biology, Honduras, Parasitology, medicine.drug
Abstract

Malaria continues to be an important health problem in Honduras despite major progress achieved reducing its incidence in the last two decades. In a context of case reduction, continuing surveillance of parasite diversity and drug resistance is an important component to assist effective malaria control strategies and support risk assessments. In this study, we employed next generation sequencing on collected Plasmodium vivax and P. falciparum samples from the Hospital Escuela (University Hospital) in Honduras between 2005 and 2017. Hospital Escuela is the main public health hospital in Honduras and receives suspected malaria cases from endemic regions within the country. The resulting sequencing data was used to assess complexity of infections, parasite population structure, parasite diversity and drug resistance profiling. All P. vivax samples and all autochtonous P. falciparum samples were monoclonal and presented a low intra population diversity (π = 0.25 and 0.07, respectively). Genotyping of drug resistance markers showed that three P. falciparum samples presented the chloroquine resistant haplotype SVMNT on pfcrtr (positions 72–76). Epidemiological data suggested that two of these samples were imported cases from Africa whereas the third one was a local case. Three suspected imported cases (two of which were also pfcrt mutants) presented the pfmdr1 86Y mutation that further enhances the CQ resistant genotype. No evidence was found for kelch13 artemisinin resistance associated mutations nor parasite genetic background mutations. Discriminant analysis of principal components and phylogenetic analysis showed two P. vivax and two P. falciparum parasite sub-populations with limited recombination between them. It also confirmed the closer relationship of the three imported cases with African strains. Our findings showed that local Honduras P. falciparum strains do not hold CQ resistance polymorphisms which aligns with clinical data reported by the country and supports the continuity of CQ based treatment in Honduras. In addition, our findings highlight the need of using genomic approaches to provide key information about parasite biology including drug resistance, population structure and HRP2/HRP3 deletions which are becoming relevant as the country move towards elimination.

Published
2020

9. First Report of Trypanosoma cruzi Infection in Salivary Gland of Bats from the Peruvian Amazon

Author

O. Melisa Del Alcazar, Christian Albujar, Luis A. Gomez-Puerta, Fredy E. Villena, V. Alberto Laguna-Torres, Sarah Blythe Ballard, Sergio Recuenco, Jorge L. Maguiña, Erik J. Jhonston, and Julia S. Ampuero

Subjects
Male, 0301 basic medicine, Chagas disease, Trypanosoma cruzi, 030231 tropical medicine, 030106 microbiology, Zoology, Salivary Glands, 03 medical and health sciences, 0302 clinical medicine, Chiroptera, Virology, Peru, parasitic diseases, medicine, Animals, Parasite hosting, Salivary gland, biology, Transmission (medicine), Articles, medicine.disease, biology.organism_classification, Infectious Diseases, medicine.anatomical_structure, Diaemus youngi, Female, Parasitology, Sylvatic cycle, Trypanosomiasis
Abstract

In the Americas, 8 million people are infected with Chagas disease, and an additional 90 million people are at risk for infection. Little is known about the role bats play in the sylvatic transmission cycle of Trypanosoma cruzi, the parasite causing Chagas disease. Here, we captured bats in the villages of Palmiche, Pachacutec, Nuevo San Martin, and Mayuriaga located in the Datem del Marañon Province in Loreto, Peru. Venous blood samples were collected by cardiac puncture or from the upper extremities, and trypanosomatids were identified by microscopy and molecularly. We collected blood samples from 121 bats on filter paper for molecular studies and 111 slides for microscopic examination of thin and thick blood smears from 16 different bat species. The prevalence of trypanosomatids in all bats species was 34.7% (42/121) and the prevalence of T. cruzi was 4.1% (5/121). In hematophagous bat species, the prevalence of trypanosomatids and T. cruzi was 36.9% (27/73) and 2.7% (2/73), respectively. In non-hematophagous bats, the prevalences of trypanosomatids and T. cruzi were 31.2% (15/48) and 6.2% (3/48), respectively. Also, we confirm the presence of T. cruzi in salivary glands of hematophagous bats Diaemus youngi. These results suggest a sylvatic cycle of trypanosomatid transmission in which bats may harbor infectious T. cruzi parasites that could be transmitted to humans via hematophagous bat bites or salivary contamination by non-hematophagous bats of vegetables consumed by humans.

Published
2018

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