Improvement of immune functions in HIV infection by sulfur supplementation: Two randomized trials

Improvement of immune functions in HIV infection by sulfur supplementation: Two randomized trials

To determine the therapeutic effect of sulfur amino acid supplementation in HIV infection we randomized 40 patients with antiretroviral therapy (ART; study 1) and 29 patients without ART (study 2) to treatment for 7 months with N-acetyl-cysteine or placebo at an individually adjusted dose according...

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Veröffentlicht in:Journal of molecular medicine (Berlin, Germany) Germany), 2000-01, Vol.78 (1), p.55-62
Hauptverfasser: Breitkreutz, Raoul, Pittack, Nicole, Nebe, Carl, Schuster, Dieter, Brust, Jürgen, Beichert, Matthias, Hack, Volker, Daniel, Volker, Edler, Lutz, Dröge, Wulf
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Albumin
Human immunodeficiency virus
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container_start_page 55
container_title Journal of molecular medicine (Berlin, Germany)
container_volume 78
creator Breitkreutz, Raoul
Pittack, Nicole
Nebe, Carl
Schuster, Dieter
Brust, Jürgen
Beichert, Matthias
Hack, Volker
Daniel, Volker
Edler, Lutz
Dröge, Wulf
description To determine the therapeutic effect of sulfur amino acid supplementation in HIV infection we randomized 40 patients with antiretroviral therapy (ART; study 1) and 29 patients without ART (study 2) to treatment for 7 months with N-acetyl-cysteine or placebo at an individually adjusted dose according to a defined scheme. The main outcome measures were the change in immunological parameters including natural killer (NK) cell and T cell functions and the viral load. Both studies showed consistently that N-acetyl-cysteine causes a marked increase in immunological functions and plasma albumin concentrations. The effect of N-acetyl-cysteine on the viral load, in contrast, was not consistent and may warrant further studies. Our findings suggest that the impairment of immunological functions in HIV super(+) patients results at least partly from cysteine deficiency. Because immune reconstitution is a widely accepted aim of HIV treatment, N-acetyl-cysteine treatment may be recommended for patients with and without ART. Our previous report on the massive loss of sulfur in HIV-infected subjects and the present demonstration of the immunoreconstituting effect of cysteine supplementation indicate that the HIV-induced cysteine depletion is a novel mechanism by which a virus destroys the immune defense of the host and escapes immune elimination.
doi_str_mv 10.1007/s001099900073
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subjects Albumin
Human immunodeficiency virus
title Improvement of immune functions in HIV infection by sulfur supplementation: Two randomized trials
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