HIV Infection Clinical Trial
Official title:
Studies on the Interaction Between HIV Infection, Lymphatic Filariasis and Diethylcarbamazine
The impact of lymphatic filariasis (LF) on HIV is assessed by measuring HIV viral load before and after DEC treatment of filariasis in double-infected individuals. The impact of HIV on lymphatic filariasis is assessed by measuring the success of DEC treatment on W. bancrofti antigenaemia and microfilaraemia in double-infected individuals. The effect of DEC treatment in individuals with lymphatic filariasis and/or HIV is assessed by measuring the pre- and post-treatment level of HIV viral load, immunological responses and micronutritional parameters, including antioxidants and markers of oxidative stress, in single- or double-infected individuals. The study is carried out as an anonymous, unlinked and double-blind placebo controlled study with cross-over design. The study groups comprise: 1) 18 double-infected individuals (HIV+/LF+), 2) 16 HIV infected individuals (HIV+/LF-) and 3) 25 individuals with lymphatic filariasis (HIV-/LF+). Based on stratified, blocked randomisation the study participants receive DEC treatment or placebo. Pre- and post-treatment (1 week, 12 weeks and 24 weeks post-treatment) blood samples are collected and analysed for HIV viral load, CD4+ T cell count, distinctive Th1 and Th2 cytokines, circulating filarial antigens (CFA), micronutrient status, antioxidant enzymes and markers of oxidative stress. After 12 weeks the study participants get the opposite treatment and post-treatment blood samples are collected four times with the same intervals as above.
Previous studies on the interaction between HIV and helminth infections have indicated that
HIV may have a negative impact on helminth infections and vice versa, and there is evidence
that treatment of chronic helminth infections in HIV infected individuals can delay the
progression of HIV. These interactions may be related to changes in the immunological
responsiveness or through an effect on reactive oxygen compounds resulting in oxidative
stress. Oxidative stress may be a neglected determinant for progression of lymphatic
filariasis and may also impair immune functions and lead to increased HIV replication
through activation of nuclear transcription factors. The present study examines the
three-way interaction between HIV infection, lymphatic filariasis caused by the helminth
parasite W. bancrofti and the drug diethylcarbamazine (DEC). DEC is an important drug for
treatment of lymphatic filariasis and previous findings indicate that DEC may also have an
effect on retroviral infections.
The impact of lymphatic filariasis (LF) on HIV is assessed by measuring HIV viral load
before and after DEC treatment of filariasis in double-infected individuals. The impact of
HIV on lymphatic filariasis is assessed by measuring the success of DEC treatment on W.
bancrofti antigenaemia and microfilaraemia in double-infected individuals. The effect of DEC
treatment in individuals with lymphatic filariasis and/or HIV is assessed by measuring the
pre- and post-treatment level of HIV viral load, immunological responses and
micronutritional parameters, including antioxidants and markers of oxidative stress, in
single- or double-infected individuals. The study is carried out as an anonymous, unlinked
and double-blind placebo controlled study with cross-over design. The study groups comprise:
1) 18 double-infected individuals (HIV+/LF+), 2) 16 HIV infected individuals (HIV+/LF-) and
3) 25 individuals with lymphatic filariasis (HIV-/LF+). Based on stratified, blocked
randomisation the study participants receive DEC treatment or placebo. Pre- and
post-treatment (1 week, 12 weeks and 24 weeks post-treatment) blood samples are collected
and analysed for HIV viral load, CD4+ T cell count, distinctive Th1 and Th2 cytokines,
circulating filarial antigens (CFA), micronutrient status, antioxidant enzymes and markers
of oxidative stress. After 12 weeks the study participants get the opposite treatment and
post-treatment blood samples aree collected four times with the same intervals as above.
If treatment of coexisting helminth infections, including lymphatic filariasis, delays the
progression of HIV, such treatment may be an important measure to alleviate the effect of
the AIDS epidemic in Africa and other areas where HIV and helminths coexist. For lymphatic
filariasis in particular such information will be of high significance in the strategic
planning by decision-makers within the ongoing international efforts for control of
lymphatic filariasis.
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Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Crossover Assignment, Masking: Double-Blind, Primary Purpose: Treatment
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