Genome Wide Linkage Study, Using a 250K SNP Map, of Plasmodium falciparum Infection and Mild Malaria Attack in a Senegalese Population

Milet, Jacqueline; Nuel, Grégory; Watier, Laurence; Courtin, David; Slaoui, Yousri; Senghor, Paul; Migot-Nabias, Florence; Gaye, Oumar; Garcia, André

doi:10.1371/journal.pone.0011616

Cited by 38 publications

(27 citation statements)

References 79 publications

(103 reference statements)

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“…Asymptomatic parasite density was also linked to chromosome 5q31 in a study from Senegal [126]. A genomewide linkage study revealed three strongly suggestive lines of evidence for linkage between mild malaria attacking both the 6p25.1 and the 12q22 regions and between the 20p11q11 region and the prevalence of parasite density in asymptomatic Senegalese children [127]. Furthermore, in this study, one gene associated with malaria infection in the 5q31–q33 was also detected, confirming the importance of this genetic region in the susceptibility to malaria infection [127].…”

Section: Immune Responsementioning

confidence: 99%

The Host Genetic Diversity in Malaria Infection

Mendonça

Gonçalves

Barral‐Netto

2012

Journal of Tropical Medicine

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Populations exposed to Plasmodium infection develop genetic mechanisms of protection against severe disease. The clinical manifestation of malaria results primarily from the lysis of infected erythrocytes and subsequent immune and inflammatory responses. Herein, we review the genetic alterations associated with erythrocytes or mediators of the immune system, which might influence malaria outcome. Moreover, polymorphisms in genes related to molecules involved in mechanisms of cytoadherence and their influence on malaria pathology are also discussed. The results of some studies have suggested that the combinatorial effects of a set of genetic factors in the erythrocyte-immunology pathway might be relevant to host resistance or susceptibility against Plasmodium infection. However, these results must be interpreted with caution because of the differences observed in the functionality and frequency of polymorphisms within different populations. With the recent advances in molecular biology techniques, more robust studies with reliable data have been reported, and the results of these studies have identified individual genetic factors for consideration in preventing severe disease and the individual response to treatment.

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Section: Immune Responsementioning

confidence: 99%

The Host Genetic Diversity in Malaria Infection

Mendonça

Gonçalves

Barral‐Netto

2012

Journal of Tropical Medicine

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“…It should be stressed, however, that we did not found linkage of IgG levels to chromosome 5q31-q33, which contains numerous genes encoding cytokines, and which was linked to parasitaemia. 3,4,[25][26][27][28] Thus, it seems that genetic variation within IL4, IL5 and IL13 genes located within chromosome 5q31-q33 does not markedly alter the levels of IgG and IgG subclasses against P. falciparum antigens in our study population, although those genes are known to be involved in antibody production, and although IL4 polymorphism was associated to antimalarial IgG levels. 21 In the same way, we did not find, in the chromosomal regions linked to IgG phenotypes, any genes encoding the cytokines known to be involved in isotype switching or B cell proliferation and differentiation, such as IL6, IL10 or IFNγ.…”

Section: Discussionmentioning

confidence: 58%

“…2,22 In other populations, ABO blood group genes located within chromosome 9q34 were associated with parasitemia and severe malaria, 23,24 whereas chromosome 12q22 was linked to mild malaria in a Senegalese population. 3 Because the antibody levels may depend on the exposure to parasite antigens, we further assessed the linkage of IgG and IgG subclass levels to the chromosomal regions of interest when taking into account parasitemia; the analyses yielded very similar results, ruling out the possibility of false linkage results due to this confounding factor. All together, these results suggest that some loci controlling the production of IgG or IgG subclasses may control parasitemia or mild malaria.…”

Section: Discussionmentioning

confidence: 99%

“…Several candidate genes have been associated with resistance against clinical malaria or parasitaemia, 1 whereas genome-wide scans mapped several loci controlling mild malaria and/or parasitaemia. [2][3][4] Furthermore, cellular and humoral responses have been shown to be associated with enhanced resistance against malaria, 5 and to be genetically controlled. 6 Anti-P. falciparum immunoglobulin G (IgG0 antibodies) are thought to have a critical role in immune protection against asexual blood stages of the parasite.…”

Section: Introductionmentioning

confidence: 99%

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Genome-wide significant linkage to IgG subclass responses against Plasmodium falciparum antigens on chromosomes 8p22-p21, 9q34 and 20q13

et al. 2014

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A genome-wide scan was conducted for the levels of total immunoglobulin G (IgG) and IgG subclasses directed against Plasmodium falciparum antigens in an urban population living in Burkina Faso. Non-parametric multipoint linkage analysis provided three chromosomal regions with genome-wide significant evidence (logarithm of the odds (LOD) score >3.6), and five chromosomal regions with genome-wide suggestive evidence (LOD score >2.2). IgG3 levels were significantly linked to chromosomes 8p22-p21 and 20q13, whereas IgG4 levels were significantly linked to chromosome 9q34. In addition, we detected suggestive linkage of IgG1 levels to chromosomes 18p11-q12 and 18q12-q21, IgG4 levels to chromosomes 1p31 and 12q24 and IgG levels to chromosome 6p24-p21. Moreover, we genotyped genetic markers located within the regions of interest in a rural population living in Burkina Faso. We detected genome-wide significant and suggestive linkage results when combining the two study populations for chromosomes 1p31, 6p24-p21, 8p22-p21, 9q34, 12q24 and 20q13. Because high anti-parasite IgG3 and low anti-parasite IgG4 levels were associated with malaria resistance, the chromosomal regions linked to IgG3 and IgG4 levels are of special interest. Although the results should be confirmed in an independent population, they may provide new insights in understanding both the genetic control of IgG production and malaria resistance.

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“…to determine the incidence or prevalence of clinical malaria in an area or in a population under close medical surveillance) clinical malaria is often considered as any case of fever or fever-related symptoms (headache, vomiting, subjective sensation of fever) associated with a P. falciparum parasite/leukocyte ratio higher than an age-dependent pyrogenic threshold of PD previously identified in the patient [43], [44]. In this case, a feverish individual harboring a PD under his age-specific threshold is not considered as a malaria case and will be monitored by the medical team involved in the study.…”

Section: Discussionmentioning

confidence: 99%

Statistical Properties of Parasite Density Estimators in Malaria

Hammami

Garcia

2013

PLoS ONE

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Malaria is a global health problem responsible for nearly one million deaths every year around 85% of which concern children younger than five years old in Sub-Saharan Africa. In addition, around million clinical cases are declared every year. The level of infection, expressed as parasite density, is classically defined as the number of asexual parasites relative to a microliter of blood. Microscopy of Giemsa-stained thick blood films is the gold standard for parasite enumeration. Parasite density estimation methods usually involve threshold values; either the number of white blood cells counted or the number of high power fields read. However, the statistical properties of parasite density estimators generated by these methods have largely been overlooked. Here, we studied the statistical properties (mean error, coefficient of variation, false negative rates) of parasite density estimators of commonly used threshold-based counting techniques depending on variable threshold values. We also assessed the influence of the thresholds on the cost-effectiveness of parasite density estimation methods. In addition, we gave more insights on the behavior of measurement errors according to varying threshold values, and on what should be the optimal threshold values that minimize this variability.

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Genome Wide Linkage Study, Using a 250K SNP Map, of Plasmodium falciparum Infection and Mild Malaria Attack in a Senegalese Population

Cited by 38 publications

References 79 publications

The Host Genetic Diversity in Malaria Infection

The Host Genetic Diversity in Malaria Infection

Genome-wide significant linkage to IgG subclass responses against Plasmodium falciparum antigens on chromosomes 8p22-p21, 9q34 and 20q13

Statistical Properties of Parasite Density Estimators in Malaria

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