Jozef Anné
Catholic University of Leuven
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Malaria Journal | 2010
Peter Van den Eede; Gert Van der Auwera; Christopher Delgado; Tine Huyse; Veronica E Soto-Calle; Dionicia Gamboa; Tanilu Grande; Hugo Rodriguez; Alejandro Llanos; Jozef Anné; Annette Erhart; Umberto D'Alessandro
BackgroundPeru is one of the Latin American countries with the highest malaria burden, mainly due to Plasmodium vivax infections. However, little is known about P. vivax transmission dynamics in the Peruvian Amazon, where most malaria cases occur. The genetic diversity and population structure of P. vivax isolates collected in different communities around Iquitos city, the capital of the Peruvian Amazon, was determined.MethodsPlasmodium vivax population structure was determined by multilocus genotyping with 16 microsatellites on 159 P. vivax infected blood samples (mono-infections) collected in four sites around Iquitos city. The population characteristics were assessed only in samples with monoclonal infections (n = 94), and the genetic diversity was determined by calculating the expected heterozygosity and allelic richness. Both linkage disequilibrium and the genetic differentiation (θ) were estimated.ResultsThe proportion of polyclonal infections varied substantially by site (11% - 70%), with the expected heterozygosity ranging between 0.44 and 0.69; no haplotypes were shared between the different populations. Linkage disequilibrium was present in all populations (IAS 0.14 - 0.61) but was higher in those with fewer polyclonal infections, suggesting inbreeding and a clonal population structure. Strong population differentiation (θ = 0.45) was found and the Bayesian inference cluster analysis identified six clusters based on distinctive allele frequencies.ConclusionThe P. vivax populations circulating in the Peruvian Amazon basin are genetically diverse, strongly differentiated and they have a low effective recombination rate. These results are in line with the low and clustered pattern of malaria transmission observed in the region around Iquitos city.
PLOS ONE | 2011
Peter Van den Eede; Veronica E Soto-Calle; Christopher Delgado; Dionicia Gamboa; Tanilu Grande; Hugo Rodriguez; Alejandro Llanos-Cuentas; Jozef Anné; Umberto D'Alessandro; Annette Erhart
Background There is an increasing body of literature reporting treatment failure of the currently recommended radical treatment of Plasmodium vivax infections. As P. vivax is the main malaria species outside the African continent, emerging tolerance to its radical treatment regime could have major consequences in countries like Peru, where 80% of malaria cases are due to P. vivax. Here we describe the results of a 1-year longitudinal follow up of 51 confirmed P. vivax patients living around Iquitos, Peruvian Amazon, and treated according to the Peruvian national guidelines. Methodology Each month a blood sample for microscopy and later genotyping was systematically collected. Recent exposure to infection was estimated by detecting antibodies against the P. vivax circumsporozoite protein (CSP) and all PCR confirmed P. vivax infections were genotyped with 16 polymorphic microsatellites. Results During a 1-year period, 84 recurrent infections, 22 positive also by microscopy, were identified, with a median survival time to first recurrent infection of 203 days. Most of them (71%) were asymptomatic; in 13 patients the infection persisted undetected by microscopy for several consecutive months. The genotype of mostly recurrent infections differed from that at day 0 while fewer differences were seen between the recurrent infections. The average expected heterozygosity was 0.56. There was strong linkage disequilibrium (IAsu200a=u200a0.29, p<1.10−4) that remained also when analyzing only the unique haplotypes, suggesting common inbreeding. Conclusion In Peru, the P. vivax recurrent infections were common and displayed a high turnover of parasite genotypes compared to day 0. Plasmodium vivax patients, even when treated according to the national guidelines, may still represent an important parasite reservoir that can maintain transmission. Any elimination effort should consider such a hidden reservoir.
Archive | 1999
Lieve Van Mellaert; Jozef Anné
Archive | 2005
Lieve Van Mellaert; Jan Theys; Oliver Pennington; Sofie Barbé; Sandra Nuyts; William Landuyt; Philippe Lambin; Nigel P. Minton; Jozef Anné
Archive | 2006
Carlos Vallin; Elsa Pimienta; Astrid Ramos; Caridad Rodríguez; Lieve Van Mellaert; Jozef Anné
Archive | 2003
Nick Geukens; Filip Frederix; E Reekmans; Elke Lammertyn; Lieve Van Mellaert; Wim Dehaen; Guido Maes; Jozef Anné
Archive | 2013
Jeroen Bouvin; S. Cajot; Pieter-Jan D'Huys; Jerry Ampofo-Asiama; Jozef Anné; Jan Van Impe; Annemie Geeraerd; Kristel Bernaerts
Proceedings of EuroPM2012 - PM Biomaterials | 2012
Annabel Braem; Lieve Van Mellaert; Dorien Hofmans; Evelien De Waelheyns; Jozef Anné; Jan Schrooten; Jef Vleugels
Archive | 2012
Annabel Braem; Lieve Van Mellaert; Dorien Hofmans; Jozef Anné; Bram Neirinck; Jan Schrooten; Jef Vleugels
Archive | 2011
Monica Sarzo; Jony Jones; Julio C. Ayala; Caridad Rodríguez; Elsa Pimienta; Mt Milanés; Carlos Vallin; Lieve Van Mellaert; Jozef Anné; Kris Huygen