Malaria Clinical Trial
Official title:
Efficacy of Chloroquine and Primaquine for the Treatment of Plasmodium Vivax Malaria in Cruzeiro do Sul, Acre, Brazil
Background: The World Health Organization recommends that antimalarial treatment policies be
evaluated every few years to check their efficacy. P. vivax malaria is the most common
species in Brazil and cases are concentrated in the Amazon Region in Brazil.
Objectives: Assess the efficacy of chloroquine and primaquine for the treatment of P. vivax
infections in Cruzeiro do Sul, Acre, Brazil.
Methods: An in vivo drug efficacy study will be conducted in Cruzeiro do Sul, Acre State,
Brazil. At least 117 study participants ≥5 years of age with parasitologically confirmed P.
vivax monoinfections will be treated under supervision with chloroquine (CQ) for three days
at a daily dose of approximately 25 mg/Kg in accordance with the Brazilian National Malaria
Control guidelines. For patients with normal glucose 6 phosphate dehydrogenase activity
levels, investigators will add primaquine at dose of 0.5mg/Kg per day for 7 days. Clinical
and parasitologic parameters will be monitored over a 28-day follow-up period to evaluate
drug efficacy and for a total period of 168 days (6 months) to evaluate chances of
recrudescence, relapse, or reinfection. Blood samples will be taken to measure the CQ levels
in blood on Day 7 and day of failure, if occurring in the initial 28 days of follow up. In
addition, a blood sample will be collected on filter paper on first day and on day of
suspected failure to help differentiate parasite genotypes using techniques based on
polymerase chain reaction. Results from this drug efficacy study will be used to assist the
Brazilian Ministry of Health in assessing their national malaria treatment policy for P.
vivax malaria.
Background The impact of malaria on the health and economic development of human populations
is greatest in the tropics and subtropics. The World Health Organization (WHO) has estimated
216 million episodes of malaria in 2010, of which 174 million (81%) were in Africa. There
were a total of 655,000 malaria deaths worldwide, approximately 86% of which in children
under 5 years of age (WHO 2011). Although the majority of deaths occur among children in
sub-Saharan Africa, malaria accounts for considerable morbidity in the Americas, particularly
in the Amazon Basin.
Most countries in the Americas have adopted the WHO Global Strategy for Malaria Control,
which relies on prompt and effective antimalarial treatment as the major means of reducing
malaria morbidity and mortality (WHO 2008). The ultimate success of this strategy rests on
the ability of ministries of health to provide antimalarial drugs with proven efficacy.
Although a wide variety of methods have been used to assess resistance to antimalarial drugs
in vivo methods, in vitro drug sensitivity testing, and molecular analyses, most national
malaria control programs rely on data from in vivo efficacy trials to assess the efficacy of
the current first- and second-line drugs and to decide if charges in malaria treatment policy
are needed.
The most widely used approach to conduct in vivo drug efficacy trials in the Americas follows
the guidelines of the WHO (WHO 2009) with the modifications recommended by the Pan American
Health Organization for studies in the Americas (PAHO 2003). The goal of such studies is to
assess antimalarial drugs currently being used for first-line treatment of uncomplicated
malaria. Much of the effort to monitor antimalarial efficacy in the Americas has been done as
part of the Amazon Network of Antimalarial Resistance Monitoring and the Amazon Malaria
Initiative (PAHO 2012). This information is critical for guiding the development of rational
antimalarial drug policies in endemic areas.
Chloroquine-resistant P. vivax was first reported from Papua New Guinea in 1989 in two
Australian soldiers (Rieckmann, Davis et al. 1989). In 1995, a study in Irian Jaya, Indonesia
showed resistance in at least 44% of the P. vivax patients treated with chloroquine (CQ)
(Baird, Basri et al. 1995). Several investigators have reported cases of CQ-resistant P.
vivax in South America. In 1996, in Guyana, Phillips et al. reported three patients in whom
25 mg/kg of CQ failed to eliminate parasitemia despite adequate therapeutic blood levels of
CQ (Phillips, Keystone et al. 1996). Three years later, in the Brazilian Amazon region,
Alecrim et al. reported a 12-year old girl with P. vivax malaria who continued to have
parasitemia after receiving a supervised course of 25mg/kg of CQ (Alecrim, Alecrim et al.
1999). More recently, Soto et al. reported three cases of CQ-resistant P. vivax in Colombia
(Soto, Toledo et al. 2001). In these last two studies, CQ blood levels were not measured and
it is not possible to confirm that adequate therapeutic levels were achieved.
Because of the serious public health implications of CQ-resistant P. vivax in the Americas,
it is critically important to limit reports to well-confirmed cases. In most cases, this will
require measurement of CQ blood levels and genotyping of parasites from the initial infection
and any suspected recrudescence. P. falciparum in vivo trials take advantage of
well-established molecular markers that help differentiate cases of recrudescence and
reinfection, by polymerase chain reaction (PCR) techniques. Although no universally accepted
technique for this purpose exists for P. vivax, investigators plan to use the
microsatellites, base pair repeats in the parasite genome, described by Imwong et al (Imwong,
Sudimack et al. 2006). Investigators believe that having PCR-corrected analysis is especially
important in the context of the long follow-up period, six months, investigators aim for this
study.
Many malaria cases in the Americas are reported in Brazil (Silveira 2001; Oliveira-Ferreira,
Lacerda et al. 2010). In 2011, 293,701 malaria cases were reported to the Brazilian National
Reportable Disease Information System. Most of these cases (99.7%) occurred in the Amazon
region, which encompasses the states of Acre, Amazonas, Amapa, Para, Maranhao, Mato Grosso,
Roraima, Rondonia, and Tocantins. In this region, socio-economic and environmental
conditions, such as presence of natural breeding sites and abundance of Anopheles mosquitoes,
favor malaria transmission. Amazonas, Rondonia, Para, and Acre states were responsible for
85.5% of malaria cases in 2011 according to the Brazilian National Reportable Disease
Information System. As in other regions of the world, malaria is seasonal in Brazil, cases
increase during or after the rainy season (Costa 2009).
In 2011, 87,6% of malaria cases in Brazil were due to P. vivax alone, 11,3% to P. falciparum
alone, and approximately 1.1% due to mixed infections with these two species. P. malariae is
rarely seen in Brazil. Acre state saw a huge increase in malaria cases from 2003 to 2004 and
from 2004 to 2005, 153% and 63%, respectively(Cesario and Cesario 2006). The Acre
municipalities of Cruzeiro do Sul, Rodrigues Alves, and Mancio Lima municipalities were
responsible for 67.7% of malaria cases in the state in 2006, when a malaria epidemic took
place in this region. Table 1 shows the absolute number of malaria cases in Brazil and Acre
state and their respective annual parasitologic index (API), which is the number of positive
malaria slides per 1,000 residents per year.
Although currently there is no evidence of CQ-resistant P. vivax in Cruzeiro do Sul, Acre
State, Brazil, the Ministry of Health would like to assess the efficacy of CQ and primaquine
for the treatment of uncomplicated P. vivax malaria as part their effort to study
antimalarial drug resistance within the country. This practice is in accordance with current
WHO recommendations (WHO 2009).
Objectives
- To assess the therapeutic efficacy of CQ and primaquine for the treatment of P. vivax
malaria in Cruzeiro do Sul, Acre State, Brazil.
- Estimate recrudescence and reinfection rates of P. vivax infection after parasite
clearance with CQ and primaquine.
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