Literature DB >> 21620959

Leishmania-macrophage interactions: insights into the redox biology.

Tim Van Assche1, Maartje Deschacht, Raquel A Inocêncio da Luz, Louis Maes, Paul Cos.   

Abstract

Leishmaniasis is a neglected tropical disease that affects about 350 million individuals worldwide. The protozoan parasite has a relatively simple life cycle with two principal stages: the flagellated mobile promastigote living in the gut of the sandfly vector and the intracellular amastigote within phagolysosomal vesicles of the vertebrate host macrophage. This review presents a state-of-the-art overview of the redox biology at the parasite-macrophage interface. Although Leishmania species are susceptible in vitro to exogenous superoxide radical, hydrogen peroxide, nitric oxide, and peroxynitrite, they manage to survive the endogenous oxidative burst during phagocytosis and the subsequent elevated nitric oxide production in the macrophage. The parasite adopts various defense mechanisms to cope with oxidative stress: the lipophosphoglycan membrane decreases superoxide radical production by inhibiting NADPH oxidase assembly and the parasite also protects itself by expressing antioxidant enzymes and proteins. Some of these enzymes could be considered potential drug targets because they are not expressed in mammals. In respect to antileishmanial therapy, the effects of current drugs on parasite-macrophage redox biology and its involvement in the development of drug resistance and treatment failure are presented.
Copyright © 2011 Elsevier Inc. All rights reserved.

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Year:  2011        PMID: 21620959     DOI: 10.1016/j.freeradbiomed.2011.05.011

Source DB:  PubMed          Journal:  Free Radic Biol Med        ISSN: 0891-5849            Impact factor:   7.376


  70 in total

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Authors:  Claudia N Paiva; Marcelo T Bozza
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2.  Molecular Cloning and Biochemical Characterization of Iron Superoxide Dismutase from Leishmania braziliensis.

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3.  Human classical monocytes control the intracellular stage of Leishmania braziliensis by reactive oxygen species.

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4.  Techniques to study phagocytosis and uptake of Leishmania tarentolae by J774 macrophages.

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5.  Upregulation of Cysteine Synthase and Cystathionine β-Synthase Contributes to Leishmania braziliensis Survival under Oxidative Stress.

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Review 7.  Immunopathogenesis of non-healing American cutaneous leishmaniasis and progressive visceral leishmaniasis.

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8.  Augmentation of antileishmanial efficacy of miltefosine in combination with tuftsin against experimental visceral leishmaniasis.

Authors:  Nishi Shakya; Shraddha A Sane; Wahajul Haq; Suman Gupta
Journal:  Parasitol Res       Date:  2012-03-06       Impact factor: 2.289

9.  A new ABC half-transporter in Leishmania major is involved in resistance to antimony.

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