Nitric oxide in Tanzanian children with malaria: inverse relationship between malaria severity and nitric oxide production/nitric oxide synthase type 2 expression.

Anstey, Nicholas M.; Weinberg, J. Brice; Hassanali, M Y; Mwaikambo, Esther D.; Manyenga, D; Misukonis, Mary A.; Arnelle, Derrick R.; Hollis, Donna; McDonald, Malcolm; Granger, Donald L.

doi:10.1084/jem.184.2.557

Cited by 386 publications

(323 citation statements)

References 54 publications

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“…Most studies to date have associated inducible NO production in the mammalian host with anti-parasitic effects (Rockett et al, 1991, Naotunne et al, 1993, Mellouk et al, 1994, Anstey et al, 1996, Pino et al, 2004, Sharma et al, 2004 as well as with increased inflammatory pathology to the host Cowden, 2003 andRiley et al, 2006). In contrast, two studies have concluded that higher levels of NO in humans (Hobbs et al, 2002) and in mice (Gramaglia et al, 2006) were associated with less severe malaria but no differences in parasitemia levels.…”

Section: Resultsmentioning

confidence: 90%

“…Nitric oxide has also been linked to the development of cerebral malaria, the most severe form of human infection, with most studies reporting a positive association between high NO levels and increased pathology in late stage disease (Clark and Cowden 2003). In contrast, Anstey et al, (1996) documented that high NO levels were associated with reduced malaria severity and low parasite density and Hobbs et al, (2002) showed that higher NO production was associated with less severe malaria but with no differences in parasitemia levels. As such, studies of NO levels in human malaria have revealed both protective and pathological effects.…”

Section: Introductionmentioning

confidence: 86%

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Low levels of mammalian TGF-β1 are protective against malaria parasite infection, a paradox clarified in the mosquito host

Luckhart

Lieber

Singh

et al. 2008

Experimental Parasitology

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Nitric oxide (NO), derived from catalysis of inducible NO synthase (iNOS), limits malaria parasite growth in mammals. Transforming growth factor (TGF)-β1 suppresses iNOS in cells in vitro as well as in vivo in mice, but paradoxically severe malaria in humans is associated with low levels of TGF-β1. We hypothesized that this paradox is a universal feature of infection and occurs in the mosquito Anopheles stephensi, an invertebrate host for Plasmodium that also regulates parasite development with inducible NO synthase (AsNOS). We show that exogenous human TGF-β1 dose-dependently regulates mosquito AsNOS expression and that parasite killing by low dose TGF-β1 depends on AsNOS catalysis. Furthermore, induction of AsNOS expression by TGF-β1 is regulated by NO synthesis. These results suggest that TGF-β1 plays similar roles during parasite infection in mammals and mosquitoes and that this role is linked to the effects of TGF-β1 on inducible NO synthesis. .

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Section: Resultsmentioning

confidence: 90%

Section: Introductionmentioning

confidence: 86%

Low levels of mammalian TGF-β1 are protective against malaria parasite infection, a paradox clarified in the mosquito host

Luckhart

Lieber

Singh

et al. 2008

Experimental Parasitology

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“…38 However, increased expression of NOS2 in PBMC, and particularly in monocytes, 39 leading to increased NOS2-derived NO synthesis, is associated with protection against clinical disease. 40 It seems therefore too early to establish a definitive causal association between NOS2 polymorphisms and malaria susceptibility.…”

Section: Discussionmentioning

confidence: 99%

Human genetic factors related to susceptibility to mild malaria in Gabon

Migot-Nabias¹,

Mombo²,

Luty³

et al. 2000

Genes Immun

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Several human genetic factors, including red blood cell polymorphisms (ABO blood group, sickle-cell trait, G6PD deficiency) as well as point mutations in the mannose binding protein (MBP) and in the promoter regions of both the TNF-␣ and NOS2 genes, influence the severity of disease due to infection with Plasmodium falciparum. We assessed their impact on mild P. falciparum malaria, as part of a longitudinal investigation of clinical, parasitological and immunological parameters in a cohort of 300 Gabonese schoolchildren. We found the following frequencies: blood group O (0.54), sicklecell trait (0.23), G6PD deficiency (0.09), MBP gene mutations (0.34), TNF-␣ promoter mutations (at positions −238: 0.17 and −308: 0.22) and NOS2 promoter mutation (0.18). Blood group O or hemoglobin AA were associated with protection against higher parasitemia. Girls with normal G6PD enzyme activity were protected against clinical malaria attacks. In addition, we demonstrated for the first time that the mutation at position −238 of the gene coding for the promoter region of TNF-␣ was positively correlated with the level of the antibody response specific for epitopes of the antigens MSA-2 and RAP-1 of P. falciparum. Genes and Immunity (2000) 1, 435-441.

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“…Nitric oxide (NO), which has been shown to be produced at higher levels by mononuclear cells in asymptomatic children [96], can suppress the pathogenesis of severe malaria through induction of heme oxygenase-1 (HO-1), CO production, and inhibition of T cell activation [97]. However, conflicting results have questioned the role for NO in mediating tolerance [98].…”

Section: Production Of Anti-inflammatory Moleculesmentioning

confidence: 99%

Malaria Parasites in the Asymptomatic: Looking for the Hay in the Haystack

Galatas

Bassat

Mayor

2016

Trends in Parasitology

108

116

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With malaria elimination back on the international agenda, programs face the challenge of targeting all Plasmodium infections, not only symptomatic cases. As asymptomatic individuals are unlikely to seek treatment, they are missed by passive surveillance while remaining infectious to mosquitoes, thus acting as silent reservoirs of transmission. To estimate the risk of asymptomatic infections in various phases of malaria elimination, we need a deeper understanding of the underlying mechanisms favoring carriage over disease, which may involve both pathogen and host factors. Here we review our current knowledge on the determinants leading to Plasmodium falciparum symptomless infections. Understanding the host-pathogen interactions that are most likely to affect transitions between malaria disease states could guide the development of tools to tackle asymptomatic carriers in elimination settings. Being AsymptomaticPeaceful coexistence with the infected host, rarely causing clinical symptoms, is a common but poorly understood phenomenon that occurs for many human pathogens [1]. Because such asymptomatic cases of infection occur without eventual overt symptoms, they do not come to clinical attention, thus representing a large hidden reservoir of active infection that permits their persistence and eventual spread to other human hosts. This is the case for many malaria infections in semi-immune individuals from endemic areas, which commonly cause a mild febrile illness or no apparent symptoms at all, while keeping parasite numbers at low densities [2] (Box 1).Carriage of asymptomatic malaria (see Glossary) infections, being at the same time difficult to detect and to manage, has considerable implications for the design and use of malaria elimination strategies. Symptomless infections that persist during the dry season in areas of seasonal transmission have been suggested to seed the malaria outbreaks after annual rains when mosquitoes reappear [3]. Similarly, asymptomatic parasitemia may potentially contribute to persistence of transmission in low-transmission settings [4]. However, the precise contribution of asymptomatic malaria to transmission in areas that have achieved substantial reductions in the malaria burden remains a matter of debate [5], as is the assumption that detecting and targeting these individuals for radical treatment, as opposed to using mass drug administration approaches, would be an efficient and effective tactic. Moreover, eradication in Europe, North America, and other parts of the world using no better diagnostics than microscopy [6] suggest that key determinants of success might not be finding the last parasite. From a practical point of view, the proportion of asymptomatic infections in certain situations and phases of malaria elimination may impose the need for modifications of detection methods (active versus passive case detection) [7] if, for example, symptom-based surveillance at health facilities is insufficient and mass blood surveys are necessary to inform the design of elimination i...

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Nitric oxide in Tanzanian children with malaria: inverse relationship between malaria severity and nitric oxide production/nitric oxide synthase type 2 expression.

Cited by 386 publications

References 54 publications

Low levels of mammalian TGF-β1 are protective against malaria parasite infection, a paradox clarified in the mosquito host

Low levels of mammalian TGF-β1 are protective against malaria parasite infection, a paradox clarified in the mosquito host

Human genetic factors related to susceptibility to mild malaria in Gabon

Malaria Parasites in the Asymptomatic: Looking for the Hay in the Haystack

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