Vivax Malaria Clinical Trial
Official title:
Estimating the Risk of Plasmodium Vivax Relapses in Afghanistan
This is an open label two-arm randomized prospective study of two treatments for P. vivax
malaria. Patients meeting study inclusion criteria will be enrolled and allocated either
chloroquine alone or chloroquine plus primaquine (0.25mg/kg/day for 14 days). Patients will
be followed-up for 1 year, with clinical and laboratory examinations at each visit. Patients
with recurrent P. vivax infection will be treated with the same medication as initially
randomized unless contraindicated. Recurrences in the two arms will be compared to estimate
the risk of and mean duration to relapse, classify the relapse pattern as early or late
relapse and to estimate the efficacy and safety of the study drugs.
Polymerase Chain Reaction (PCR) analysis will be used as far as possible help to distinguish
between relapse and re-infection. Samples for chloroquine pharmacokinetic analysis will be
collected on day 7 from each study subject as well as on the day of recurrence if within 8
weeks of chloroquine
Globally more than 100 countries are endemic of malaria and about 60% of world population are
at risk of getting the infection while around 10% are harboring malaria parasite in their
blood stream. Of the four species of plasmodium that infect humans, Plasmodium vivax is
responsible for 50% of all malaria cases outside Africa, and is endemic in the Middle East,
Asia and Western Pacific, with a lower prevalence in Central and South America a common cause
of malaria in many tropical and subtropical regions. Conventional control methods are rather
inefficient for preventing transmission of this species of malaria. This is partly due to the
persistence of the infectious reservoir, which take the form of latent hypnozoites in the
liver, producing recurrent relapses and opportunities for new transmission for several years
after initial infection.
Primaquine (PQ) is the only available drug regimen which can eliminate the persisting liver
stages (hypnozoites) of P. vivax,but its use for 14 days is ineffective to prevent relapses
at 15 mg daily dose (0.25mg/kg) in Southeast Asia and in Brazil, and at a higher dose of 22.5
mg daily in the Southwest Pacific. Due to high relapse rates, a primaquine regimen of 30 mg
daily (0.5 mg/kg) for 14 d is now widely recommended for glucose-6-phosphate dehydrogenase
(G6PD) normal patients.
P.vivax is the predominant species in Pakistan and eastern Afghanistan. In this area G6PD
deficiency is a common trait (7% in Pakistani and 14% in Afghan Pashtoon respectively).
However facilities to test for G6PD deficiency are not available and hence routine
administration of primaquine is not recommended in national guidelines because of the risk of
severe haemolysis in those who cannot be tested.
Several national malaria programmes in Asia have adopted a truncated 5-day course of PQ for
vivax malaria to reduce the risk of haemolysis to reasonable levels and to increases
compliance rates. Recently this has been documented as being ineffective at reducing relapse
rates amongst Afghan refugees in Pakistan while a supervised 14 day course can significantly
reduce the frequency of second and third episodes of disease. This is also confirmed by a
study in India. Use of the 14 day course is only recommended where the G6PD status of the
individual is known, and, currently, where compliance with the full course can be assured.
However supervision of patients for 14 day post presentation is seldom feasible in the
majority of settings where vivax malaria predominates. Therefore the supposition that
patients in a low literacy population will not comply with a 14 day course of treatment in
the absence of supervision needs to be confirmed under normal operational conditions.
Compliance in taking the drug cannot be monitored by direct observation or by chemical assay
of residues in the blood because such interference may, in itself, affect compliance.
;
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