Malaria Clinical Trial
Official title:
Impact of Antimalarial Treatment on Measures of T Cell Suppression/Regulation in Healthy Adults From Ouelessebougou, Mali
Background:
Malaria is a disease that affects many people in the country of Mali and other parts of
Africa. It is caused by germs that are spread by mosquito bites. Malaria may be mild, but can
also be serious or can lead to death if not diagnosed and treated promptly. Children younger
than 5 years and pregnant women are at highest risk of malaria. Researchers want to better
understand how malaria infection suppresses the immune system. They want to compare a group
of adults who receive antimalarial treatment to a group that does not receive it.
Objective:
To investigate the effect of antimalarial treatment at the beginning of the dry season on the
immune system and malaria episodes.
Eligibility:
Healthy adults ages 18-60 who live in the area of Doneguebougou, Mali.
Design:
Participants will be screened with a physical exam and health questions.
If participants are found to be sick at the screening visit, they will get initial care at
the study clinic free of charge. They may get referrals for consultation.
Participants will be randomly assigned to a group. One group will get an approved
antimalarial drug called Coartem . The other will not receive it.
Participants in the Coartem group will take the drug for 3 days.
All participants will have blood tests.
Al participants will be seen about once a month for about 1 year. At each visit, they will be
asked how they are feeling and be examined. Blood will be drawn.
If participants become sick at any time, they will come to the clinic to be examined.
Malaria, caused by Plasmodium falciparum, is a devastating disease that causes significant
mortality and morbidity both directly and indirectly in endemic regions. Lower all-cause
mortality in children under five years of age have resulted from better malaria transmission
control measures in endemic regions.
It has been seen in multiple studies that malaria infection, including asymptomatic carriage,
suppresses or modulates the immune system; how exactly this suppression is achieved is
unclear. Currently, efforts to develop long-lasting, effective vaccines to combat malaria
have not been successful. One of the impediments of concern is poor immune response to the
vaccine candidates. Understanding the immunomodulatory effects of malaria infection to
vaccine responses and to subsequent malaria infection is thus key in these efforts.
In order to further understand how the presence of parasitemia may modulate the immune
system, we propose to study the effects of treating a portion of adult volunteers with a
treatment course of artemether/lumefantrine (Coartem ) at the beginning of the dry season
(approximately January) in Ouelessebougou, Mali to clear parasitemia carriage during the dry
season and following them for the next 10-12 months through an entire dry and wet season. We
will enroll 50% blood smear or polymerase chain reaction (PCR) positive volunteers and
distribute them equally into two groups at the beginning of the dry season, those who receive
or do not receive antimalarial treatment. These subjects will then be followed monthly
throughout the dry and rainy seasons to determine the effect of this treatment on T cell
markers of suppression/regulation and the incidence of asymptomatic malaria infection and
clinical malaria. We hypothesize that markers of T cell suppression/regulation throughout the
dry season will be lower in adults who receive a single pre-emptive treatment with Coartem .
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