Malaria Clinical Trial
Official title:
Pharmacokinetics of Chlorproguanil-Dapsone in Pregnant Women With Plasmodium Falciparum Infection, and Reinfection With P. Falciparum During Pregnancy Following Treatment
NCT number | NCT00126971 |
Other study ID # | CDC-NCID-4341 |
Secondary ID | |
Status | Suspended |
Phase | Phase 1 |
First received | August 3, 2005 |
Last updated | August 14, 2006 |
Start date | July 2005 |
Controlling malaria during pregnancy is a vital strategy in decreasing maternal and child
mortality in Africa. There are data from clinical trials and program evaluations in stable
transmission areas that show that intermittent preventive treatment (IPT) with two doses of
sulfadoxine-pyrimethamine (SP) is safe, efficacious, and effective in preventing maternal
anemia, placental parasitemia, and low birth weight (LBW). SP is also the first-line drug
for the case-management of malaria in pregnancy. Resistance to SP, however, is increasing
rapidly in East and Central Africa and compliance to the rescue treatment, 7-days of oral
quinine, is low. There is an urgent need to find effective, safe and practical alternative
drugs for the treatment of malaria in pregnancy. The synergistic antifolate combination
chlorproguanil-dapsone (CD), has recently become available. It is inexpensive, well
tolerated, is given as single daily treatment doses for 3 days, and is effective in the
treatment of drug-resistant falciparum malaria.
The investigators propose a small pharmacokinetic study of CD to determine if current fixed
combination CD tablets provide an adequate dosage in pregnancy. Such a study is a necessary
precursor to any large Phase II trials to further evaluate the safety and efficacy of CD for
use in pregnant women. To accomplish this, a group of 66 parasitemic pregnant women in this
open label trial will receive CD and be sampled by venipuncture at two of the seven
follow-up visits scheduled for pharmacokinetic analyses, such that 11 patients are sampled
at each of 12 time points. To serve as a reference, 66 non-pregnant women with symptomatic
malaria will also be treated with CD and will have identical pharmacokinetic (PK) analyses
performed.
Pregnant women greater than or equal to 20 weeks gestation with P. falciparum parasitemia on
peripheral blood film will be given an insecticide-treated net (ITN) and will receive CD
(1.5 or 2 tablets daily for 3 days, depending on weight). All study drug dosing will be
observed. Women will be examined, adverse events recorded, and blood samples collected at
days 0, 1, 2, 3, 7, 14, 21, and 28 after treatment, and thereafter every 14 days until
delivery. Women will be further randomized to receive additional blood draws for
pharmacokinetic analyses using a modified rich PK schedule. Each woman will only have 2
additional blood draws. Women at delivery will have peripheral and placental blood films
prepared. Newborns will be weighed, examined, and gestational age determined. Women
requiring antimalarial treatment for parasitemia at any point between enrollment and
delivery will be treated with quinine. Adverse effects will be assessed at each scheduled
visit, any sick visits during the study, and at delivery.
Status | Suspended |
Enrollment | 132 |
Est. completion date | |
Est. primary completion date | |
Accepts healthy volunteers | No |
Gender | Female |
Age group | 15 Years to 49 Years |
Eligibility |
Inclusion Criteria: For the pregnancy part of the study, a subject will be considered eligible for inclusion in this study only if all of the following criteria apply: She - Is pregnant and presents at the antenatal clinic (ANC) facilities of the study hospital. - Has uncomplicated malaria (either symptomatic or not) with pure (on microscopic grounds) P falciparum parasitemia. - Has a gestational age of >= 20 and < 36 weeks (defined by fundal height). - Is willing and able to participate and comply with the study protocol, attend the ANCs regularly and agrees to supervised drug delivery. - Has no history of antimalarial intake in the previous 4 weeks, with the exception of chloroquine or quinine. - Has given written or witnessed verbal consent. For the 66 non-pregnant women, the following inclusion criteria will apply: - Has uncomplicated malaria (either symptomatic or not) with pure (on microscopic grounds) P falciparum parasitemia. - Negative urine pregnancy test. - Is willing and able to participate and comply with the study protocol, attend the ANCs regularly and agrees to supervised drug delivery. - Has no history of antimalarial intake in the previous 4 weeks, with the exception of chloroquine or quinine. - Has given written or witnessed verbal consent. Exclusion Criteria: - Any feature of severe malaria. - A history of convulsions during the present illness. - Known history of G6PD deficiency or sickle cell disease. - Other conditions requiring hospitalization or evidence of severe concomitant infection at time of presentation. - Women on daily cotrimoxazole prophylaxis - Use of any antimalarial (other than chloroquine or quinine) in the past 4 weeks. - Known chronic disease (cardiac, renal, hepatic, hemoglobinopathy), or known hepatic or renal impairment. - Inability to follow the ANC consultation. - Hemoglobin < 7 g/dL (will be measured before enrollment) - Inability to tolerate oral treatment reflected by persistent vomiting of the study drugs. - Known allergy to either the study drugs, or to any sulfa-containing medications. - Age <15 years. - Age >49 years. |
Allocation: Non-Randomized, Endpoint Classification: Pharmacokinetics Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
Country | Name | City | State |
---|---|---|---|
Mali | Faladje Missionary Dispensary | Faladje |
Lead Sponsor | Collaborator |
---|---|
Centers for Disease Control and Prevention | Liverpool School of Tropical Medicine, Malaria Research and Training Center, Bamako, Mali |
Mali,
Keuter M, van Eijk A, Hoogstrate M, Raasveld M, van de Ree M, Ngwawe WA, Watkins WM, Were JB, Brandling-Bennett AD. Comparison of chloroquine, pyrimethamine and sulfadoxine, and chlorproguanil and dapsone as treatment for falciparum malaria in pregnant and non-pregnant women, Kakamega District, Kenya. BMJ. 1990 Sep 8;301(6750):466-70. — View Citation
Mutabingwa T, Nzila A, Mberu E, Nduati E, Winstanley P, Hills E, Watkins W. Chlorproguanil-dapsone for treatment of drug-resistant falciparum malaria in Tanzania. Lancet. 2001 Oct 13;358(9289):1218-23. Erratum in: Lancet 2001 Nov 3;358(9292):1556. — View Citation
Winstanley P, Watkins W, Muhia D, Szwandt S, Amukoye E, Marsh K. Chlorproguanil/dapsone for uncomplicated Plasmodium falciparum malaria in young children: pharmacokinetics and therapeutic range. Trans R Soc Trop Med Hyg. 1997 May-Jun;91(3):322-7. — View Citation
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Pharmacokinetic analyses of pregnant women taking CD | |||
Secondary | Proportion of pregnant women sleeping under ITNs who become re-infected with malaria before delivery following administration of a single dose of CD for P. falciparum parasitemia | |||
Secondary | Proportion of treatment failures by day 28 following initial treatment | |||
Secondary | Treatment failure will be defined according to standard WHO criteria for low to moderate transmission areas to account for fact that some pregnant women are asymptomatic | |||
Secondary | Early treatment failure: development of danger signs or severe malaria on Day 1, Day 2 or Day 3 in the presence of parasitemia (severe malaria defined by altered sensorium convulsions | |||
Secondary | persistent vomiting | |||
Secondary | renal impairment | |||
Secondary | respiratory distress) | |||
Secondary | a fall in Hb below 5g/dl anytime | |||
Secondary | parasitemia on Day 2 higher than Day 0 count irrespective of axillary temperature | |||
Secondary | parasitemia on Day 3 with axillary temperature >= 37.5 °C | |||
Secondary | parasitemia on Day 3 >= 25% of count on Day 0 | |||
Secondary | Late clinical failure: development of danger signs of severe malaria after Day 3 in the presence of parasitemia, without previously meeting any of the criteria of early treatment failure | |||
Secondary | presence of parasitemia and axillary temperature >= 37.5 °C on any day from Day 4 (inclusive) to Day 28 (inclusive), without previously meeting any of the criteria of early treatment failure | |||
Secondary | Late parasitological failure: parasitemia on any day between Day 7 (inclusive) and Day 28 (inclusive) | |||
Secondary | axillary temperature <37.5 °C without previously meeting any of the criteria of early treatment failure or late clinical failure, after exclusion of re-infection by PCR (days | |||
Secondary | adequate clinical and parasitological response [ACPR] will be defined as: absence of parasitemia on Day 28 irrespective of axillary temperature without previously meeting any of the criteria of early treatment failure | |||
Secondary | or late clinical failure | |||
Secondary | or late parasitologic failure) | |||
Secondary | Parasite clearance by Day 3 | |||
Secondary | Mean Hb concentrations by Day 28, and hematological recovery by day 28 (Hb > 11 g/dL) | |||
Secondary | Gametocytemia | |||
Secondary | Maternal parasitemia at delivery | |||
Secondary | Placental malaria parasitemia | |||
Secondary | Mean birth weight and gestational age of newborn | |||
Secondary | Presence of congenital abnormalities | |||
Secondary | Incidence of fetal loss | |||
Secondary | Incidence of perinatal and neonatal mortality, assessed 4-6 weeks after due date of delivery | |||
Secondary | Incidence of fetal death, defined as absence of fetal heartbeat | |||
Secondary | Hypoglycemia requiring treatment | |||
Secondary | Other adverse events during treatment period (up to 28 days) |
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