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Differences in pathogenicity and virulence of Trypanosoma brucei gambiense field isolates in experimentally infected Balb/C mice.
Kaboré, Jacques; Camara, Oumou; Koffi, Mathurin; Sanou, Djénéba; Ilboudo, Hamidou; Sakandé, Hassane; Camara, Mamadou; De Meeûs, Thierry; Ravel, Sophie; Belem, Adrien Marie Gaston; MacLeod, Annette; Bucheton, Bruno; Jamonneau, Vincent; Thévenon, Sophie.
Afiliación
  • Kaboré J; Centre International de Recherche-Développement sur l'Elevage en zone Subhumide (CIRDES), 01 BP 454, Bobo-Dioulasso 01, Burkina Faso; Université NAZI BONI de Bobo-Dioulasso, UFR Sciences et Techniques, 01 BP 1091, Bobo-Dioulasso 01, Burkina Faso. Electronic address: jacqueskabore@yahoo.fr.
  • Camara O; Programme National de Lutte contre la THA, BP 851, Conakry, Guinea. Electronic address: oumicam@yahoo.fr.
  • Koffi M; Université Jean Lorougnon Guédé, UFR Environnement, BP 150, Daloa, Côte d'Ivoire. Electronic address: m9koffi@yahoo.fr.
  • Sanou D; Université NAZI BONI de Bobo-Dioulasso, UFR Sciences et Techniques, 01 BP 1091, Bobo-Dioulasso 01, Burkina Faso. Electronic address: sanoudjeneba164@yahoo.fr.
  • Ilboudo H; Programme National de Lutte contre la THA, BP 851, Conakry, Guinea. Electronic address: hamidou_ilboudo@hotmail.com.
  • Sakandé H; Centre International de Recherche-Développement sur l'Elevage en zone Subhumide (CIRDES), 01 BP 454, Bobo-Dioulasso 01, Burkina Faso. Electronic address: sakhass@yahoo.fr.
  • Camara M; Programme National de Lutte contre la THA, BP 851, Conakry, Guinea. Electronic address: mamadycamarafr@yahoo.fr.
  • De Meeûs T; INTERTRYP, Univ Montpellier, CIRAD, IRD, Montpellier, France. Electronic address: thierry.demeeus@ird.fr.
  • Ravel S; INTERTRYP, Univ Montpellier, CIRAD, IRD, Montpellier, France. Electronic address: sophie.ravel@ird.fr.
  • Belem AMG; Université NAZI BONI de Bobo-Dioulasso, UFR Sciences et Techniques, 01 BP 1091, Bobo-Dioulasso 01, Burkina Faso. Electronic address: belemadrien@yahoo.fr.
  • MacLeod A; Wellcome Center for Molecular Parasitology, University of Glasgow, 464 Bearsden Road, Glasgow G60 1QH, UK. Electronic address: Annette.macleod@glasgow.ac.uk.
  • Bucheton B; INTERTRYP, Univ Montpellier, CIRAD, IRD, Montpellier, France. Electronic address: bruno.bucheton@ird.fr.
  • Jamonneau V; INTERTRYP, Univ Montpellier, CIRAD, IRD, Montpellier, France. Electronic address: vincent.jamonneau@ird.fr.
  • Thévenon S; CIRAD, UMR INTERTRYP, F-34398 Montpellier, France. Electronic address: sophie.thevenon@cirad.fr.
Infect Genet Evol ; 63: 269-276, 2018 09.
Article en En | MEDLINE | ID: mdl-29807131
ABSTRACT
Trypanosoma brucei gambiense (T. b. gambiense) is the major causative agent of human African trypanosomiasis (HAT). A great variety of clinical outcomes have been observed in West African foci, probably due to complex host-parasite interactions. In order to separate the roles of parasite genetic diversity and host variability, we have chosen to precisely characterize the pathogenicity and virulence of T. b. gambiense field isolates in a mouse model. Thirteen T. b. gambiense strains were studied in experimental infections, with 20 Balb/C infected mice per isolate. Mice were monitored for 30 days, in which mortality, parasitemia, anemia, and weight were recorded. Mortality rate, prepatent period, and maximum parasitemia were estimated, and a survival analysis was performed to compare strain pathogenicity. Mixed models were used to assess parasitemia dynamics, weight, and changes in Packed Cell Volume (PCV). Finally, a multivariate analysis was performed to infer relationships between all variables. A large phenotypic diversity was observed. Pathogenicity was highly variable, ranging from strains that kill their host within 9 days to a non-pathogenic strain (no deaths during the experiment). Virulence was also variable, with maximum parasitemia values ranging from 42 million to 1 billion trypanosomes/ml. Reduced PCV and weight occurred in the first two weeks of the infection, with the exception of two strains. Finally, the global analysis highlighted three groups of strains a first group with highly pathogenic strains showing an early mortality associated with a short prepatent period; a second group of highly virulent strains with intermediate pathogenicity; and a third group of isolates characterized by low pathogenicity and virulence patterns. Such biological differences could be related to the observed clinical diversity in HAT. A better understanding of the biological pathways underlying the observed phenotypic diversity could thus help to clarify the complex nature of the host-parasite interactions that determine the resistance/susceptibility status to T. brucei gambiense.
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Texto completo: 1 Base de datos: MEDLINE Asunto principal: Fenotipo / Trypanosoma brucei gambiense / Tripanosomiasis Africana / Parasitemia / Interacciones Huésped-Parásitos Tipo de estudio: Prognostic_studies País/Región como asunto: Africa Idioma: En Revista: Infect Genet Evol Asunto de la revista: BIOLOGIA / DOENCAS TRANSMISSIVEIS / GENETICA Año: 2018 Tipo del documento: Article
Texto completo
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Texto completo: 1 Base de datos: MEDLINE Asunto principal: Fenotipo / Trypanosoma brucei gambiense / Tripanosomiasis Africana / Parasitemia / Interacciones Huésped-Parásitos Tipo de estudio: Prognostic_studies País/Región como asunto: Africa Idioma: En Revista: Infect Genet Evol Asunto de la revista: BIOLOGIA / DOENCAS TRANSMISSIVEIS / GENETICA Año: 2018 Tipo del documento: Article