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Tahar Rachida, Ringwald Pascal, Basco Leonardo. (2009). Molecular epidemiology of malaria in Cameroon. XXVIII. In vitro activity of dihydroartemisinin against clinical isolates of Plasmodium falciparum and sequence analysis of the P. falciparum ATPase 6 gene. American Journal of Tropical Medicine and Hygiene, 81 (1), 13-18. ISSN 0002-9637.

Titre du document
Molecular epidemiology of malaria in Cameroon. XXVIII. In vitro activity of dihydroartemisinin against clinical isolates of Plasmodium falciparum and sequence analysis of the P. falciparum ATPase 6 gene
Année de publication
2009
Type de document
Article référencé dans le Web of Science WOS:000267526500004
Auteurs
Tahar Rachida, Ringwald Pascal, Basco Leonardo
Source
American Journal of Tropical Medicine and Hygiene, 2009, 81 (1), 13-18 ISSN 0002-9637
The Plasmodium falciparum ATPase 6 (Pfatp6), homolog of sarco-endoplasmic reticulum, calcium-dependent ATPase in malaria parasites, has been proposed to be the main target of artemisinins. Four distinct point mutations (L263E, E431K, A623E, and S769N) have been reported to be associated with artemisinin resistance. ne Pfatp6 sequence polymorphism was determined to evaluate the prevalence of these mutations in fresh clinical isolates in Yaounde, Cameroon, and compare sequence data with in vitro response to dihydroartemisinin. Two major haplotypes were observed: the wild-type LEAS (n = 60, 62%) and a single mutant LKAS (n = 35, 36%). These amino acid substitutions did not influence the level of in vitro response to dihydroartemisinin (P > 0.05). Plasmodium falciparum isolates from Cameroon are highly sensitive in vitro to artemisinins. However, the relatively high prevalence of E431K may be a warning signal that warrants a regular monitoring of these molecular markers and/or in vitro activity of artemisinin derivatives.
Plan de classement
Epidémiologie générale [050EPID] ; Lutte [052ANOPAL04]
Description Géographique
CAMEROUN
Localisation
Fonds IRD [F B010046224]
Identifiant IRD
fdi:010046224
Contact