Falciparum Malaria Clinical Trial
Official title:
The Impact of Artemether-Lumefantrine on Genes Associated With Antimalarial Resistance in an Area of Seasonal Transmission
The newly introduced antimalarial drug artemether-lumefantrine is currently recommended as second line antimalarial in Sudan. Recurrent infection after treatment with this drug has been associated with selection of certain genes in the malaria parasite. However there is no information on this association in Sudan.This study is going to look into the genetics of resistance to artemether-lumefantrine.
In Sudan the current treatment protocol includes two artemisinin combinations (ACT);
artesunate + sulphadoxine/pyrimethamine (AS/SP) as first line and artemether-lumefantrine
(AL) as second line. This protocol has been implemented in 2004, since then various studies
have reported the high efficacy of both combinations (e.g. Adam et al., 2005; Elamin et al.,
2005; Mohamed et al., 2006).
However, there has been no report of the impact of these combinations on drug resistance
markers in Sudan. Data from other African countries has shown that AL selects for certain
alleles in the pfmdr-1 gene (Sisowath et al., 2005, Dokomajilar et al., 2006; Humphreys et
al., 2007), but the impact on the prevalence of different pfcrt and pfmdr-1alleles remains
unclear. It is essential to monitor ACT efficacy in addition to identify molecular markers
that are associated with response to different drugs to facilitate epidemiological surveys
for evidence based decision making. Recent work in The Gambia suggests that
transmission-related endpoints, such as emergence of gametocytes after treatment, may be
better indicators of emerging drug resistance (Hallett et al., 2006).
The aim of the proposed study is to examine the impact of treatment with
artemether-lumefantrine (AL) on alleles of pfcrt and pfmdr-1 in P. falciparum isolates in an
area of marked seasonal transmission in eastern Sudan. Most studies of resistance markers
measure marker prevalence by DNA amplification, but we will also investigate gene expression
using quantitative amplification of mRNA encoding pfcrt and pfmdr-1. The impact of genotype
and gene expression levels on treatment outcome, and on the emergence and density of
peripheral gametocytes will be examined.
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Observational Model: Cohort, Time Perspective: Prospective
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