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3. The global response to the COVID-19 pandemic: how have immunology societies contributed?

Author

Osier, Faith, Ting, Jenny, Fraser, John, Lambrecht, Bart, Romano, Marta, Gazzinelli, Ricardo, Bortoluci, Karina, Zamboni, Dario, Akbar, Arne, Evans, Jennie, Brown, Doug, Patel, Kamala, Wu, Yuzhang, Perez, Ana, Pérez, Oliver, Kamradt, Thomas, Falk, Christine, Barda-Saad, Mira, Ariel, Amiram, Santoni, Angela, Annunziato, Francesco, Cassatella, Marco, Kiyono, Hiroshi, Chereshnev, Valeriy, Dieye, Alioune, Mbow, Moustapha, Mbengue, Babacar, Niang, Maguette, and Suchard, Melinda

Subjects
Antiviral Agents, Betacoronavirus, COVID-19, COVID-19 Vaccines, Community-Institutional Relations, Coronavirus Infections, Global Health, Humans, International Cooperation, Pandemics, Patient Education as Topic, Personal Protective Equipment, Pneumonia, Viral, SARS-CoV-2, Severe Acute Respiratory Syndrome, Societies, Scientific, Viral Vaccines
Abstract

The COVID-19 pandemic is shining a spotlight on the field of immunology like never before. To appreciate the diverse ways in which immunologists have contributed, Nature Reviews Immunology invited the president of the International Union of Immunological Societies and the presidents of 15 other national immunology societies to discuss how they and their members responded following the emergence of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2).

Published
2020

5. From Genome-wide Association Studies to Functional Variants: ARL14 Cis-regulatory Variants Are Associated With Severe Malaria.

Author

Adjemout, Mathieu, Gallardo, Frederic, Torres, Magali, Thiam, Alassane, Mbengue, Babacar, Dieye, Alioune, Marquet, Sandrine, and Rihet, Pascal

Subjects
GENOME-wide association studies, LINKAGE disequilibrium, REPORTER genes, SINGLE nucleotide polymorphisms, T cells
Abstract

Background Genome-wide association studies have identified several nonfunctional tag single-nucleotide polymorphisms (SNPs) associated with severe malaria. We hypothesized that causal SNPs could play a significant role in severe malaria by altering promoter or enhancer activity. Here, we sought to identify such regulatory SNPs. Methods SNPs in linkage disequilibrium with tagSNPs associated with severe malaria were identified and were further annotated using FUMA. Then, SNPs were prioritized using the integrative weighted scoring method to identify regulatory ones. Gene reporter assays were performed to assess the regulatory effect of a region containing candidates. The association between SNPs and severe malaria was assessed using logistic regression models in a Senegalese cohort. Results Among 418 SNPs, the best candidates were rs116525449 and rs79644959, which were in full disequilibrium between them, and located within the ARL14 promoter. Our gene reporter assay results revealed that the region containing the SNPs exhibited cell-specific promoter or enhancer activity, while the SNPs influenced promoter activity. We detected an association between severe malaria and those 2 SNPs using the overdominance model and we replicated the association of severe malaria with the tagSNP rs116423146. Conclusions We suggest that these SNPs regulate ARL14 expression in immune cells and the presentation of antigens to T lymphocytes, thus influencing severe malaria development. [ABSTRACT FROM AUTHOR]

Published
2024
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8. Evidence for an ancient BRCA1 pathogenic variant in inherited breast cancer patients from Senegal

Author

Ndiaye, Rokhaya, Diop, Jean Pascal Demba, Bourdon-Huguenin, Violaine, Dem, Ahmadou, Diouf, Doudou, Dieng, Mamadou Moustapha, Diop, Pape Saloum, Kane Gueye, Serigne Modou, Ba, Seydi Abdoul, Dia, Yacouba, Ka, Sidy, Mbengue, Babacar, Thiam, Alassane, Sylla Niang, Maguette, Gueye, Papa Madieye, Faye, Oumar, Lopez Sall, Philomene, Cisse, Aynina, Diop, Papa Amadou, Sobol, Hagay, and Dieye, Alioune

Published
2020
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9. Genetic contribution of breast cancer genes in women of black African origin.

Author

Ndiaye, Rokhaya, Diop, Pascal Demba, Dem, Ahmadou, and Dieye, Alioune

Subjects
BLACK Africans, BREAST cancer, BREAST, BRCA genes, GENETIC variation, CHECKPOINT kinase 2
Abstract

Breast cancer (BC) is an increasing public health issue worldwide. BC incidence and mortality rates are rising in transitioning countries in Africa, with the most rapid increase occurring in Sub-Saharan Africa (SSA). Female BC represents 25.8% of all cancer diagnosis in SSA. Early age at onset, high grade and triple negative tumors are hallmarks of BC in this region, associated with germline pathogenic variants in susceptibility genes. While several genes have been associated with genetic predisposition (BRCA1, BRCA2, PALB2, TP53, PTEN, CDH1, STK11, ATM, CHEK2, NBN, BARD1, BRIP1, RAD50, RAD51C, RAD51D, … ), most studies have reported contribution of BRCA1 and BRCA2 pathogenic variants. Genetic contribution of BRCA genes has been estimated at 27% in Caucasian women. Available data from population of African origin are scarce and have mainly focused on pathogenic variants of BRCA1 and BRCA2. Reports from main studies on large sample size highlighted that BRCA1 still the major gene associated with BC in SSA. In addition, BRCA2, PALB2, and P53, are also on the top major genes with high penetrance, associated with BC. Mutation spectrum of BC genes in black African women seems to be different from Caucasian with increasing number of founder mutations identified. We hypothesis that the genetic contribution of known BC genes may be different between women of black African origin compared to Caucasians. In this review we explore the genetic contribution of known breast cancer genes in women of African origin, and discuss perspectives for prevention and patients care strategies in the era of precision medicine. [ABSTRACT FROM AUTHOR]

Published
2023
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13. High Fecal Carriage of Extended-Spectrum β-Lactamase Producing Enterobacteriaceae by Children Admitted to the Pediatric University Hospital Complex in Bangui, Central African Republic.

Author

Sanke-Waïgana, Hugues, Fall, Cheikh, Gody, Jean-Chrysostome, Komba, Eliot Kosh, Ngaya, Gilles, Mbecko, Jean-Robert, Yambiyo, Brice Martial, Manirakiza, Alexandre, Vernet, Guy, Dieye, Alioune, and Dieye, Yakhya

Subjects
ENTEROBACTERIACEAE, TIGECYCLINE, CARBAPENEMS, KLEBSIELLA, PHENOTYPES, DRUG resistance in microorganisms
Abstract

Antimicrobial resistance (AMR) is a global public health threat. Quality data on AMR are needed to tackle the rise of multidrug-resistant clones. These data are rare in low-income countries, especially in sub-Saharan Africa. In this study, we investigated the rise of extended-spectrum β-lactamase–producing (ESBL) Enterobacteriaceae in Bangui, Central African Republic. We collected 278 fecal samples from 0–5-year-old children admitted to the Pediatric University Hospital Complex in Bangui from July to September 2021. Enterobacteriaceae were isolated and identified, and their susceptibility to 19 antibiotics was tested. We recovered one and two Enterobacteriaceae species from 208 and 29 samples, respectively. One clone of each species from each sample was further characterized, for a total of 266 isolates. Escherichia coli predominated, followed by Klebsiella. AMR was frequent, with 98.5% (262/266) of the isolates resistant to at least one antibiotic. Additionally, 89.5% (238/266) of the isolates were multidrug resistant, with resistance being frequent against all tested antibiotics except carbapenems and tigecycline, for which no resistance was found. Importantly, 71.2% (198/278) of the children carried at least one ESBL species, and 85.3% (227/266) of the isolates displayed this phenotype. This study confirms the rise of ESBL Enterobacteriaceae in Bangui and stresses the need for action to preserve the efficacy of antibiotics, as crucial for the treatment of bacterial infections. [ABSTRACT FROM AUTHOR]

Published
2023
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14. Galectin‐3 as a biomarker in breast neoplasms: Mechanisms and applications in patient care.

Author

Niang, Doudou Georges Massar, Gaba, Folly Mawulolo, Diouf, Adame, Hendricks, Jacobus, Diallo, Rokhaya Ndiaye, Niang, Maguette Deme Sylla, Mbengue, Babacar, and Dieye, Alioune

Subjects
BREAST tumors, GALECTINS, PATIENT care, BIOMARKERS, TUMOR microenvironment, BREAST imaging
Abstract

Galectin‐3 is a member of the lectin family encoded by the LGALS3 gene on chromosome 14. It is secreted by a wide range of immune cells and mammary tumor cells. Through its activity on the tumor microenvironment, in particular on tumor‐infiltrating leukocytes, galectin‐3 improves the proliferation, survival, and colonizing ability of mammary neoplastic cells. Consequently, galectin‐3 expression in the tumor microenvironment could worsen therapeutic outcomes of breast neoplasms and become a biomarker and a therapeutic target in combined immunotherapy in breast neoplasms. There is a limited amount of information that is available on galectin‐3 in breast cancer in Africa. In this review, we analyze how galectin‐3 influences the tumor microenvironment and its potential as a biomarker and therapeutic target in breast neoplasms. We aim to emphasize the significance of investigating galectin‐3 in breast neoplasms in Africa based on the results of studies conducted elsewhere. [ABSTRACT FROM AUTHOR]

Published
2022
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15. G6PD and HBB polymorphisms in the Senegalese population: prevalence, correlation with clinical malaria.

Author

Thiam, Fatou, Diop, Gora, Coulonges, Cedric, Derbois, Céline, Mbengue, Babacar, Thiam, Alassane, Nguer, Cheikh Momar, Zagury, Jean Francois, Deleuze, Jean-Francois, and Dieye, Alioune

Subjects
MALARIA, GENETIC polymorphisms, SENEGALESE, GLUCOSE-6-phosphate dehydrogenase deficiency, GENETIC markers, PHENOTYPIC plasticity
Abstract

Background. Host genetic factors contribute to the variability of malaria phenotypes and can allow a better understanding of mechanisms involved in susceptibility and/or resistance to Plasmodium falciparum infection outcomes. Several genetic polymorphisms were reported to be prevalent among populations living in tropical malariaendemic regions and induce protection against malaria. The present study aims to investigate the prevalence of HBB (chr11) and G6PD (chrX) deficiencies polymorphisms among Senegalese populations and their associations with the risk for severe Plasmodium falciparum malaria occurrence. Methods. We performed a retrospective study with 437 samples, 323 patients recruited in hospitals located in three different endemic areas where malaria episodes were confirmed and 114 free malaria controls. The patients enrolled were classified into two groups: severe malaria (SM) (153 patients) and uncomplicated malaria (UM) (170 patients). PCR and DNA sequencing assessed host genetic polymorphisms in HBB and G6PD. Using a multivariate regression and additive model, estimates of the impact of human HBB and G6PD polymorphisms on malaria incidence were performed. Results. Six frequent SNPs with minor allele frequencies (MAF) > 3% were detected in the HBB gene (rs7946748, rs7480526, rs10768683, rs35209591, HbS (rs334) and rs713040) and two in the G6PD gene (rs762515 and rs1050828 (G6PD-202 G > A). Analysis of selected HbS polymorphism showed significant association with protective effect against severe malaria with a significant p-value D 0.033 (OR 0.38, 95% CI [0.16≥ 0.91]) forSMvs.UMcomparison. Surprisingly, our study did not identify the protective effect of variant HbC polymorphism against severe malaria. Finally, we found some of the polymorphisms, like HbS (rs334), are associated with age and biological parameters like eosinophils, basophils, lymphocytes etc. Conclusion. Our data report HBB and G6PD polymorphisms in the Senegalese population and their correlation with severe/mild malaria and outcome. The G6PD and HBB deficiencies are widespread in West Africa endemic malaria regions such as The Gambia, Mali, and Burkina Faso. The study shows the critical role of genetic factors in malaria outcomes. Indeed, genetic markers could be good tools for malaria endemicity prognosis. [ABSTRACT FROM AUTHOR]

Published
2022
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16. Identification of ATP2B4 Regulatory Element Containing Functional Genetic Variants Associated with Severe Malaria.

Author

Nisar, Samia, Torres, Magali, Thiam, Alassane, Pouvelle, Bruno, Rosier, Florian, Gallardo, Frederic, Ka, Oumar, Mbengue, Babacar, Diallo, Rokhaya Ndiaye, Brosseau, Laura, Spicuglia, Salvatore, Dieye, Alioune, Marquet, Sandrine, and Rihet, Pascal

Subjects
GENETIC variation, MALARIA, GENOME-wide association studies, LINKAGE disequilibrium, ERYTHROCYTES, MESSENGER RNA
Abstract

Genome-wide association studies for severe malaria (SM) have identified 30 genetic variants mostly located in non-coding regions. Here, we aimed to identify potential causal genetic variants located in these loci and demonstrate their functional activity. We systematically investigated the regulatory effect of the SNPs in linkage disequilibrium (LD) with the malaria-associated genetic variants. Annotating and prioritizing genetic variants led to the identification of a regulatory region containing five ATP2B4 SNPs in LD with rs10900585. We found significant associations between SM and rs10900585 and our candidate SNPs (rs11240734, rs1541252, rs1541253, rs1541254, and rs1541255) in a Senegalese population. Then, we demonstrated that both individual SNPs and the combination of SNPs had regulatory effects. Moreover, CRISPR/Cas9-mediated deletion of this region decreased ATP2B4 transcript and protein levels and increased Ca2+ intracellular concentration in the K562 cell line. Our data demonstrate that severe malaria-associated genetic variants alter the expression of ATP2B4 encoding a plasma membrane calcium-transporting ATPase 4 (PMCA4) expressed on red blood cells. Altering the activity of this regulatory element affects the risk of SM, likely through calcium concentration effect on parasitaemia. [ABSTRACT FROM AUTHOR]

Published
2022
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17. New Insights Into c.815_824dup Pathogenic Variant of BRCA1 in Inherited Breast Cancer: A Founder Mutation of West African Origin.

Author

Diop, Jean Pascal Demba, Sène, Andréa Régina Gnilane, Dia, Yacouba, Ba, Seydi Abdoul, Mbacke, Serigne Saliou, Ly, Cheikh Ameth Tidiane, Sarr, Pierre Diaga, Diouf, Doudou, Ka, Sidy, Mbengue, Babacar, Gueye, Serigne Modou Kane, Diop, Pape Saloum, Sylla Niang, Maguette, Gueye, Papa Madieye, Lopez Sall, Philomene, Dem, Ahmadou, Cisse, Aynina, Dieye, Alioune, and Ndiaye, Rokhaya

Subjects
BRCA genes, BREAST cancer, GENETIC mutation, SLAVE trade, AFRICAN Americans
Abstract

Founder mutations have been reported in BRCA1 and BCRA2 in different ethnic groups with inherited breast cancer. Testing of targeted mutations in specific populations is important for cancer prevention in mutation carriers. In Sub-Saharan Africa, only a few studies have reported specific founder mutations in inherited breast cancer. The pathogenic variant c.815_824dup of BRCA1 has been reported as the most frequent among African American populations with inherited breast cancer and was supposed to have a West African origin. Recent report from Senegal identified this variant in women with inherited breast cancer at the highest frequency ever reported. The variant was linked to a common haplotype confirming its founder effect in West Africa. In this article, we review the mutation history of c.815_824dup and discuss how it spread out of Africa through the transatlantic slave trade. [ABSTRACT FROM AUTHOR]

Published
2022
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21. NCR3 polymorphism, haematological parameters, and severe malaria in Senegalese patients.

Author

Thiam, Alassane, Baaklini, Sabrina, Mbengue, Babacar, Nisar, Samia, Diarra, Maryam, Marquet, Sandrine, Fall, Mouhamadou Mansour, Sanka, Michel, Thiam, Fatou, Diallo, Rokhaya Ndiaye, Torres, Magali, Dieye, Alioune, and Rihet, Pascal

Subjects
MALARIA, CEREBRAL malaria, LEUKOCYTE count, PLASMODIUM falciparum, BLOOD sampling
Abstract

Background. Host factors, including host genetic variation, have been shown to influence the outcome of Plasmodium falciparum infection. Genome-wide linkage studies have mapped mild malaria resistance genes on chromosome 6p21, whereas NCR3-412 polymorphism (rs2736191) lying within this region was found to be associated with mild malaria. Methods. Blood samples were taken from 188 Plasmodium falciparum malaria patients (76 mild malaria patients, 85 cerebral malaria patients, and 27 severe non-cerebral malaria patients). NCR3-412 (rs2736191) was analysed by sequencing, and haematological parameters were measured. Finally, their association with clinical phenotypes was assessed. Results. We evidenced an association of thrombocytopenia with both cerebral malaria and severe non-cerebral malaria, and of an association of high leukocyte count with cerebral malaria. Additionally, we found no association of NCR3-412 with either cerebral malaria, severe non-cerebral malaria, or severe malaria after grouping cerebral malaria and severe non-cerebral malaria patients. Conclusions. Our results suggest that NCR3 genetic variation has no effect, or only a small effect on the occurrence of severe malaria, although it has been strongly associated with mild malaria. We discuss the biological meaning of these results. Besides, we confirmed the association of thrombocytopenia and high leukocyte count with severe malaria phenotypes. [ABSTRACT FROM AUTHOR]

Published
2018
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23. Relationship between Antibody Levels, IgG Binding to Plasmodium falciparum-Infected Erythrocytes, and Disease Outcome in Hospitalized Urban Malaria Patients from Dakar, Sénégal.

Author

Mbengue, Babacar, Fall, Mouhamadou Mansour, Sylla Niang, Maguette, Niang, Birahim, Varela, Marie Louise, Diatta, Antoine Marie, Mbow, Moustapha, Ndiaye, Kantome, Ndiaye Diallo, Rokhaya, Dieye, Alioune, and Perraut, Ronald

Subjects
ANTIGEN analysis, IMMUNOGLOBULIN analysis, ERYTHROCYTES, AGE distribution, BIOLOGICAL assay, CHI-squared test, ENZYME-linked immunosorbent assay, FLOW cytometry, HOSPITAL patients, IMMUNOGLOBULINS, EVALUATION of medical care, MALARIA, METROPOLITAN areas, PROBABILITY theory, PROTOZOA, RESEARCH funding, STATISTICS, DATA analysis, DISEASE prevalence, SEVERITY of illness index, DATA analysis software, DESCRIPTIVE statistics, PARASITEMIA, MANN Whitney U Test, PROGNOSIS
Abstract

Background. Management of clinical malaria requires the development of reliable diagnostic methods and efficient biomarkers for follow-up of patients. Protection is partly based on IgG responses to parasite antigens exposed at the surface of infected erythrocytes (iRBCs). These IgG responses appeared low during clinical infection, particularly in severe disease. Methods. We analyzed the IgG binding capacity to the surface of live erythrocytes infected by knob positive FCR3 strain. Sera from 69 cerebral malaria (CM) and 72 mild malaria (MM) cases were analyzed by ELISA for IgG responses to five antigens from iRBC and by flow cytometry for IgG binding as expressed in labeling index ratio (LIR). The relationship between IgG levels, LIR, parasitemia, age, and the clinical outcomes was evaluated. Results. We found a significant decrease of LIR in adult CM fatal cases compared to surviving patients (p=0.019). In MM, LIRs were correlated to IgG anti-iRBC and anti-PfEMP3/5 levels. In CM, no correlation was found between LIR, IgG levels, and parasitemia. Conclusion. The IgG binding assay was able to discriminate outcome of cerebral malaria cases and it deserves further development as a potential functional-associated assay for symptomatic malaria analysis. [ABSTRACT FROM AUTHOR]

Published
2016
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24. Inflammatory cytokine and humoral responses to Plasmodium falciparum glycosylphosphatidylinositols correlates with malaria immunity and pathogenesis.

Author

Mbengue, Babacar, Niang, Birahim, Niang, Maguette Sylla, Varela, Marie Louise, Fall, Becaye, Fall, Mouhamadou Mansour, Diallo, Rokhaya Ndiaye, Diatta, Bacary, Gowda, D. Channe, Dieye, Alioune, and Perraut, Ronald

Subjects
CYTOKINES, CELLULAR immunity, IMMUNOREGULATION, PLASMODIUM falciparum, PLASMODIUM
Abstract

Pro-inflammatory cytokines induced by glycosylphosphatidylinositols (GPIs) of Plasmodium falciparum contribute to malaria pathogenesis and hence, the naturally acquired anti-GPI antibody thought to provide protection against severe malaria (SM) by neutralizing the stimulatory activity of GPIs. In previous studies, the anti-GPI antibody levels increased with age in parallel with the development of acquired immunity, and high levels of anti-GPI antibodies were associated with mild malaria (MM) cases. In the present study, the relationship between the levels of pro-inflammatory cytokines and anti-GPI IgG antibody responses, parasitemia, and the clinical outcomes were evaluated in SM and mild malaria (MM) patients. Sera from a total of 110 SM and 72 MM cases after excluding of ineligible patients were analyzed for the levels of anti-GPI antibodies, IgG subclasses, and cytokine responses by ELISA. While the total anti-GPI antibody levels were similar in overall SM and MM groups, they were significantly higher in surviving SM patients than in fatal SM cases. In the case of cytokines, the TNF-α and IL-6 levels were significantly higher in SM compared to MM, whereas the IL-10 levels were similar in both groups. The data presented here demonstrate that high levels of the circulatory pro-inflammatory, TNF-α, and IL-6, are indicators of malaria severity, whereas anti-inflammatory cytokine IL-10 level does not differentiate SM and MM cases. Further, among SM patients, relatively low levels of anti-GPI antibodies are indicators of fatal outcomes compared to survivors, suggesting that anti-GPI antibodies provide some level of protection against SM fatality. [ABSTRACT FROM AUTHOR]

Published
2016
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25. Genetic Determination and Linkage Mapping of Plasmodium falciparum Malaria Related Traits in Senegal.

Author

Sakuntabhai, Anavaj, Ndiaye, Rokhaya, Casadémont, Isabelle, Peerapittayamonkol, Chayanon, Rogier, Christophe, Tortevoye, Patricia, Tall, Adama, Paul, Richard, Turbpaiboon, Chairat, Phimpraphi, Waraphon, Trape, Jean-Francois, Spiegel, André, Heath, Simon, Mercereau-Puijalon, Odile, Dieye, Alioune, and Julier, Cécile

Subjects
PLASMODIUM falciparum, MALARIA transmission, GENES, PHENOTYPES, ETHNICITY
Abstract

Plasmodium falciparum malaria episodes may vary considerably in their severity and clinical manifestations. There is good evidence that host genetic factors contribute to this variability. To date, most genetic studies aiming at the identification of these genes have used a case/control study design for severe malaria, exploring specific candidate genes. Here, we performed a family-based genetic study of falciparum malaria related phenotypes in two independent longitudinal survey cohorts, as a first step towards the identification of genes and mechanisms involved in the outcome of infection. We studied two Senegalese villages, Dielmo and Ndiop that differ in ethnicity, malaria transmission and endemicity. We performed genome-scan linkage analysis of several malaria-related phenotypes both during clinical attacks and asymptomatic infection. We show evidence for a strong genetic contribution to both the number of clinical falciparum malaria attacks and the asymptomatic parasite density. The asymptomatic parasite density showed linkage to chromosome 5q31 (LOD = 2.26, empirical p = 0.0014, Dielmo), confirming previous findings in other studies. Suggestive linkage values were also obtained at three additional chromosome regions: the number of clinical malaria attacks on chromosome 5p15 (LOD = 2.57, empirical p = 0.001, Dielmo) and 13q13 (LOD = 2.37, empirical p = 0.0014 Dielmo), and the maximum parasite density during asymptomatic infection on chromosome 12q21 (LOD = 3.1, empirical p<10-4, Ndiop). While regions of linkage show little overlap with genes known to be involved in severe malaria, the four regions appear to overlap with regions linked to asthma or atopy related traits, suggesting that common immune related pathways may be involved. [ABSTRACT FROM AUTHOR]

Published
2008
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26. ETHICS COMMITTEES IN WESTERN AND CENTRAL AFRICA: CONCRETE FOUNDATIONS.

Author

EFFA, PIERRE, MASSOUGBODJI, ACHILLE, NTOUMI, FRANCINE, HIRSCH, FRANÇOIS, DEBOIS, HENRI, VICARI, MARISSA, DERME, ASSETOU, NDEMANGA-KAMOUNE, JACQUES, NGUEMBO, JOSEPH, IMPOUMA, BENIDO, AKU, JEAN-PAUL, EHOUMAN, ARMAND, DIEYE, ALIOUNE, and KILAMA, WEN

Subjects
ETHICS committees, CLINICAL trials, RESEARCH ethics, FORUMS, CONFERENCES & conventions, AFRICANS, DEVELOPING countries
Abstract

The involvement of developing countries in international clinical trials is necessary for the development of appropriate medicines for local populations. However, the absence of appropriate structures for ethical review represents a barrier for certain countries. Currently there is very little information available on existing structures dedicated to ethics in western and central Africa. This article briefly describes historical milestones in the development of networks dedicated to capacity building in ethical review in these regions and outlines the major conclusions of two workshops on this issue, which were held in September and October 2002 in Libreville, Gabon, and Paris, France. The workshops were the culmination of collaboration between the African Malaria Network Trust (AMANET) and the Pan African Bioethics Initiative (PABIN). They produced an update on ethics organizations with regard to mission, function, activities, members, and contact people, in eight countries within the regions discussed. As a result of the commitment of mandated delegates, a further prominent outcome followed these workshops: the creation of national structures, where none existed before, dedicated to the ethical review of clinical trials. [ABSTRACT FROM AUTHOR]

Published
2007
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27. Lymphocyte response in vitro to Plasmodium falciparum merozoite antigens in donors from a holoendemic area.

Author

Dieye, Alioune, Heidrich, Hans-G., Rogier, Christophe, Trape, Jean-Francois, Launois, Pascal, Holder, Anthony, and Sarthou, Jean-Louis

Abstract

Crude merozoite antigens from Plasmodium falciparum were used to evaluate the profilerative response of peripheral mononuclear cells (PBMCs) from 114 inhabitants of the village of Dielmo (Senegal, West Africa) exposed continuously to malaria transmission. The high or low responses to merozoite antigens obtained in lymphocyte stimulation assays were correlated with the presence or absence of parasites, IFN-γ production and HLA phenotype. The high responders produced high levels of IFN-γ, in contrast to the low responders, most of whom did not secrete IFN-γ (23/27). Among others, the two HLA phenotypes HLA-B51 and HLA-DR1 were significantly associated with a high response ( P<0.05). [ABSTRACT FROM AUTHOR]

Published
1993
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30. Genetic variants of RNASE3 (ECP) and susceptibility to severe malaria in Senegalese population.

Author

Diop, Gora, Derbois, Céline, Loucoubar, Cheikh, Mbengue, Babacar, Ndao, Bineta Niakhana, Thiam, Fatou, Thiam, Alassane, Ndiaye, Rokhaya, Dieye, Yakhya, Olaso, Robert, Deleuze, Jean-Francois, and Dieye, Alioune

Subjects
MALARIA, PLASMODIUM falciparum, RIBONUCLEASES, GENETIC polymorphisms, MEDICAL genetics, PUBLIC health
Abstract

Background: Severe forms of malaria (SM) are an outcome of Plasmodium falciparum infection and can cause death especially in children under 4 years of age. RNASE3 (ECP) has been identified as an inhibitor of Plasmodium parasites growth in vitro, and genetic analysis in hospitalized Ghanaian subjects has revealed the RNASE3 +371G/C (rs2073342) polymorphism as a susceptibility factor for cerebral malaria. The +371 C allele results in an Arg/Thr mutation that abolishes the cytotoxic activity of the ECP protein. The present study aims to investigate RNASE3 gene polymorphisms and their putative link to severe malaria in a malaria cohort from Senegal. Methods/results: Patients enrolled from hospitals were classified as having either uncomplicated (UM) or severe malaria (SM). The analysis of the RNASE3 gene polymorphisms was performed in 241 subjects: 178 falciparum infected (96 SM, 82 UM) and 63 non-infected subjects as population control group (CTR). Six frequent SNPs (MAF > 3%) were identified, and one SNP was associated with malaria severity by performing a logistic regression analysis SM vs.UM: RNASE3 +499G/C (rs2233860) under age, sex as covariates and HbS/HbC polymorphisms adjustment (p = 0.003, OR 0.43, CI 95% 0.20–0.92). The polymorphisms: +371G/C (rs2073342), +499G/C (rs2233860) and +577A/T (rs8019343) defined a haplotype risk (G-G-T) for malaria severity (Fisher exact test, p = 0.03) (OR 4.1, IC 95% (1.1–14.9). Conclusion: In addition to the previously described association of +371G/C polymorphism in Ghanaians cohort, the RNASE3 +499G/C polymorphism was associated with susceptibility to SM in a Senegalese population. The haplotype +371G/+499G/+577T defined by RNASE3 polymorphisms was associated with severity. The genetic association identified independently in the Senegalese population provide additional evidence of a role of RNASE3 (ECP) in malaria severity. [ABSTRACT FROM AUTHOR]

Published
2018
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33. Evaluation of a flow cytometry method for CD4 T cell enumeration based on volumetric primary CD4 gating using thermoresistant reagents

Author

Dieye, Tandakha Ndiaye, Diaw, Papa Alassane, Daneau, Géraldine, Wade, Djibril, Sylla Niang, Maguette, Camara, Makhtar, Diallo, Abdoul Aziz, Toure Kane, Coumba, Diop Ndiaye, Halimatou, Mbengue, Babacar, Dieye, Alioune, Kestens, Luc, and Mboup, Souleymane

Subjects
*FLOW cytometry, *T cells, *VOLUMETRIC analysis, *DRUG resistance, *CD4 antigen, *CHEMICAL reagents, *HIV-positive persons, *ANTIRETROVIRAL agents
Abstract

Abstract: Laboratory follow-up of HIV patients in resource-limited settings requires appropriate instruments for CD4 T cell enumeration. In this study, we evaluated the application of a simplified, mobile and robust flow cytometry system, the Apogee Auto 40 analyzer (Auto40) using thermoresistant reagents, for CD4 T cell enumeration. We measured the absolute CD4 counts in fresh whole blood samples from 170 Senegalese subjects, including 129 HIV-positive (HIV+) patients and 41 HIV-negative (HIV−) controls. Based on volumetric primary CD4 gating, cells were stained with commercially available reagents (Easy MoAb CD4;Bio-D, Valenzano, Italy) and analyzed on the Auto40. The results were compared with those from the FACSCount system (Becton Dickinson, San Jose, USA). Repeatability analysis was performed on duplicate testing of 49 samples on both FACSCount and Auto40. The intra-run precision was measured by 10 replicates using 3 clinical blood samples with low, intermediate and high CD4 concentrations. The results from the two instruments were in good agreement. The percent similarity between the results of both instruments was 99%±relative standard deviation of 12.7%. The concordance correlation coefficient was 0.99. The absolute bias and limits of agreement (LOA) between the two instruments, calculated by Bland–Altman analysis, were clinically acceptable (bias: +4 cells/μl; LOA: −111 to +120 cells/μl). The clinical agreement between the two instruments at a cutoff of 200 CD4 cells/μl was 94%. The repeatability of measurements on the Auto40 was also similar to that observed with FACSCount system (bias +0.1 cells/μl, coefficient of variation 2.5% vs bias −1.1cells/μl, coefficient of variation 2.9% respectively). In conclusion, our results indicate that the Auto 40 system, using thermoresistant reagents, is suitable for CD4 T cell enumeration and will be a helpful tool to improve HIV laboratory monitoring in resource-limited settings. [Copyright &y& Elsevier]

Published
2011
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34. Differential antibody responses to Plasmodium falciparum glycosylphosphatidylinositol anchors in patients with cerebral and mild malaria

Author

Perraut, Ronald, Diatta, Bacary, Marrama, Laurence, Garraud, Olivier, Jambou, Ronan, Longacre, Shirley, Krishnegowda, Gowdahalli, Dieye, Alioune, and Gowda, D. Channe

Subjects
*PLASMODIUM falciparum, *IMMUNOGLOBULINS, *BRAIN diseases, *MALARIA
Abstract

Abstract: Glycosylphosphatidylinositol (GPI) membrane anchors of Plasmodium falciparum surface proteins are thought to be important factors contributing to malaria pathogenesis, and anti-GPI antibodies have been suggested to provide protection by neutralizing the toxic activity of GPIs. In this study, IgG responses against P. falciparum GPIs and a baculovirus recombinant MSP1p19 antigen were evaluated in two distinct groups of 70 patients each, who were hospitalized with malaria. Anti-GPI IgGs were significantly lower in patients hospitalized with confirmed cerebral malaria compared to those with mild malaria (P &#60; 0.01) but did not discriminate for fatal outcome. In contrast, a specific marker of the anti-parasite immunity, as monitored by the anti-MSP1p19 IgG response, was similar in both cerebral and mild malaria individuals, although it was significantly lower in a subgroup with fatal outcomes. These results are consistent with a potential anti-toxin role for anti-GPI antibodies associated with protection against cerebral malaria. [Copyright &y& Elsevier]

Published
2005
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35. COVID-19 in Africa: Dampening the storm?

Author

Mbow M, Lell B, Jochems SP, Cisse B, Mboup S, Dewals BG, Jaye A, Dieye A, and Yazdanbakhsh M

Subjects
Africa epidemiology, Age Factors, Antibodies, Neutralizing immunology, Antibodies, Viral immunology, COVID-19, Communicable Disease Control, Coronavirus Infections immunology, Coronavirus Infections prevention & control, Coronavirus Infections virology, Cytokine Release Syndrome etiology, Humans, Immunity, Cellular, Macrophages, Alveolar immunology, Pandemics prevention & control, Pneumonia, Viral immunology, Pneumonia, Viral prevention & control, Pneumonia, Viral virology, SARS-CoV-2, T-Lymphocytes immunology, Betacoronavirus genetics, Betacoronavirus immunology, Betacoronavirus pathogenicity, Coronavirus Infections epidemiology, Pneumonia, Viral epidemiology
Published
2020
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36. A Worldwide Map of Plasmodium falciparum K13-Propeller Polymorphisms.

Author

Ménard D, Khim N, Beghain J, Adegnika AA, Shafiul-Alam M, Amodu O, Rahim-Awab G, Barnadas C, Berry A, Boum Y, Bustos MD, Cao J, Chen JH, Collet L, Cui L, Thakur GD, Dieye A, Djallé D, Dorkenoo MA, Eboumbou-Moukoko CE, Espino FE, Fandeur T, Ferreira-da-Cruz MF, Fola AA, Fuehrer HP, Hassan AM, Herrera S, Hongvanthong B, Houzé S, Ibrahim ML, Jahirul-Karim M, Jiang L, Kano S, Ali-Khan W, Khanthavong M, Kremsner PG, Lacerda M, Leang R, Leelawong M, Li M, Lin K, Mazarati JB, Ménard S, Morlais I, Muhindo-Mavoko H, Musset L, Na-Bangchang K, Nambozi M, Niaré K, Noedl H, Ouédraogo JB, Pillai DR, Pradines B, Quang-Phuc B, Ramharter M, Randrianarivelojosia M, Sattabongkot J, Sheikh-Omar A, Silué KD, Sirima SB, Sutherland C, Syafruddin D, Tahar R, Tang LH, Touré OA, Tshibangu-wa-Tshibangu P, Vigan-Womas I, Warsame M, Wini L, Zakeri S, Kim S, Eam R, Berne L, Khean C, Chy S, Ken M, Loch K, Canier L, Duru V, Legrand E, Barale JC, Stokes B, Straimer J, Witkowski B, Fidock DA, Rogier C, Ringwald P, Ariey F, and Mercereau-Puijalon O

Subjects
Algorithms, Artemisinins therapeutic use, Asia, Southeastern, China, Endemic Diseases, Genotype, Humans, Lactones therapeutic use, Malaria, Falciparum drug therapy, Malaria, Falciparum parasitology, Plasmodium falciparum drug effects, Sequence Analysis, DNA, Artemisinins pharmacology, Drug Resistance genetics, Lactones pharmacology, Mutation, Plasmodium falciparum genetics, Polymorphism, Genetic, Protozoan Proteins genetics
Abstract

Background: Recent gains in reducing the global burden of malaria are threatened by the emergence of Plasmodium falciparum resistance to artemisinins. The discovery that mutations in portions of a P. falciparum gene encoding kelch (K13)-propeller domains are the major determinant of resistance has provided opportunities for monitoring such resistance on a global scale., Methods: We analyzed the K13-propeller sequence polymorphism in 14,037 samples collected in 59 countries in which malaria is endemic. Most of the samples (84.5%) were obtained from patients who were treated at sentinel sites used for nationwide surveillance of antimalarial resistance. We evaluated the emergence and dissemination of mutations by haplotyping neighboring loci., Results: We identified 108 nonsynonymous K13 mutations, which showed marked geographic disparity in their frequency and distribution. In Asia, 36.5% of the K13 mutations were distributed within two areas--one in Cambodia, Vietnam, and Laos and the other in western Thailand, Myanmar, and China--with no overlap. In Africa, we observed a broad array of rare nonsynonymous mutations that were not associated with delayed parasite clearance. The gene-edited Dd2 transgenic line with the A578S mutation, which expresses the most frequently observed African allele, was found to be susceptible to artemisinin in vitro on a ring-stage survival assay., Conclusions: No evidence of artemisinin resistance was found outside Southeast Asia and China, where resistance-associated K13 mutations were confined. The common African A578S allele was not associated with clinical or in vitro resistance to artemisinin, and many African mutations appear to be neutral. (Funded by Institut Pasteur Paris and others.).

Published
2016
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37. Cytokine response during non-cerebral and cerebral malaria: evidence of a failure to control inflammation as a cause of death in African adults.

Author

Dieye Y, Mbengue B, Dagamajalu S, Fall MM, Loke MF, Nguer CM, Thiam A, Vadivelu J, and Dieye A

Abstract

Background. With 214 million cases and 438,000 deaths in 2015, malaria remains one of the deadliest infectious diseases in tropical countries. Several species of the protozoan Plasmodium cause malaria. However, almost all the fatalities are due to Plasmodium falciparum, a species responsible for the severest cases including cerebral malaria. Immune response to Plasmodium falciparum infection is mediated by the production of pro-inflammatory cytokines, chemokines and growth factors whose actions are crucial for the control of the parasites. Following this response, the induction of anti-inflammatory immune mediators downregulates the inflammation thus preventing its adverse effects such as damages to various organs and death. Methods. We performed a retrospective, nonprobability sampling study using clinical data and sera samples from patients, mainly adults, suffering of non-cerebral or cerebral malaria in Dakar, Sénégal. Healthy individuals residing in the same area were included as controls. We measured the serum levels of 29 biomarkers including growth factors, chemokines, inflammatory and anti-inflammatory cytokines. Results. We found an induction of both pro- and anti-inflammatory immune mediators during malaria. The levels of pro-inflammatory biomarkers were higher in the cerebral malaria than in the non-cerebral malaria patients. In contrast, the concentrations of anti-inflammatory cytokines were comparable in these two groups or lower in CM patients. Additionally, four pro-inflammatory biomarkers were significantly increased in the deceased of cerebral malaria compared to the survivors. Regarding organ damage, kidney failure was significantly associated with death in adults suffering of cerebral malaria. Conclusions. Our results suggest that a poorly controlled inflammatory response determines a bad outcome in African adults suffering of cerebral malaria.

Published
2016
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38. Inflammatory cytokine and humoral responses to Plasmodium falciparum glycosylphosphatidylinositols correlates with malaria immunity and pathogenesis.

Author

Mbengue B, Niang B, Niang MS, Varela ML, Fall B, Fall MM, Diallo RN, Diatta B, Gowda DC, Dieye A, and Perraut R

Abstract

Pro-inflammatory cytokines induced by glycosylphosphatidylinositols (GPIs) of Plasmodium falciparum contribute to malaria pathogenesis and hence, the naturally acquired anti-GPI antibody thought to provide protection against severe malaria (SM) by neutralizing the stimulatory activity of GPIs. In previous studies, the anti-GPI antibody levels increased with age in parallel with the development of acquired immunity, and high levels of anti-GPI antibodies were associated with mild malaria (MM) cases. In the present study, the relationship between the levels of pro-inflammatory cytokines and anti-GPI IgG antibody responses, parasitemia, and the clinical outcomes were evaluated in SM and mild malaria (MM) patients. Sera from a total of 110 SM and 72 MM cases after excluding of ineligible patients were analyzed for the levels of anti-GPI antibodies, IgG subclasses, and cytokine responses by ELISA. While the total anti-GPI antibody levels were similar in overall SM and MM groups, they were significantly higher in surviving SM patients than in fatal SM cases. In the case of cytokines, the TNF-α and IL-6 levels were significantly higher in SM compared to MM, whereas the IL-10 levels were similar in both groups. The data presented here demonstrate that high levels of the circulatory pro-inflammatory, TNF-α, and IL-6, are indicators of malaria severity, whereas anti-inflammatory cytokine IL-10 level does not differentiate SM and MM cases. Further, among SM patients, relatively low levels of anti-GPI antibodies are indicators of fatal outcomes compared to survivors, suggesting that anti-GPI antibodies provide some level of protection against SM fatality.

Published
2015
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39. The use of crude Plasmodium falciparum antigens for comparison of antibody responses in patients with mild malaria vs. cerebral malaria.

Author

Mbengue B, Niang B, Diatta B, Tall A, Garraud O, Perraut R, and Dieye A

Subjects
Adolescent, Adult, Aged, Case-Control Studies, Female, Humans, Immunoglobulin G blood, Immunoglobulin G immunology, Immunoglobulin M blood, Immunoglobulin M immunology, Malaria, Cerebral blood, Malaria, Cerebral parasitology, Malaria, Falciparum blood, Malaria, Falciparum parasitology, Male, Merozoite Surface Protein 1 immunology, Merozoites immunology, Middle Aged, Plasmodium falciparum growth & development, Retrospective Studies, Schizonts immunology, Severity of Illness Index, Young Adult, Antibodies, Protozoan immunology, Antigens, Protozoan immunology, Malaria, Cerebral immunology, Malaria, Falciparum immunology, Plasmodium falciparum immunology
Abstract

Background: Cerebral malaria (CM) is one of the major causes of death in African populations infected with Plasmodium falciparum. Only 1% of infected subjects develop CM. The reasons for these differences are not fully understood, but it is likely that the host humoral response against blood-stage antigens plays a role in protection from malaria, although the precise targets and mechanisms mediating immunity remain unclear., Objective: The purpose of this study was to distinguish between defined P. falciparum-specific Ab response patterns in patients presenting with mild malaria (MM) vs. CM., Methods: We used a panel of P. falciparum conserved antigens including crude blood-stage extracts schizont, merozoite and parasitised erythrocyte membranes and MSP-1p19, PfEB200, R23 and GST-5 recombinant antigens in a retrospective case-control study of symptomatic adults, one group presenting confirmed CM without fatal outcome and another group with MM. We further matched P. falciparum-specific Ab responses with those from individuals living in an endemic setting known to have protective immunity and considered them as "immune control" subjects (IC). Total IgG, IgM and IgG subclass Ab responses were determined using ELISA method., Results: Substantial Ab responses were found in symptomatic patients, significantly lower than the "immune control" subjects, and with a limited quantitative difference between MM versus CM. Interestingly, asynchronous IgM response was evidenced in CM contrary to MM., Conclusion: Our results suggest that the contribution of an efficient IgG response against parasite multiplication is of importance in the evolution towards CM manifestation without fatal outcome and deserves further analysis for vaccine candidates.

Published
2010
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40. Relationship of binding of immunoglobulin G to Plasmodium falciparum-infected erythrocytes with parasite endemicity and antibody responses to conserved antigen in immune individuals.

Author

Diatta AM, Marrama L, Tall A, Trape JF, Dieye A, Garraud O, Mercereau-Puijalon O, and Perraut R

Subjects
Adolescent, Adult, Animals, Antigen-Antibody Reactions, Antigens, Protozoan, Child, Child, Preschool, Hemoglobin A, Hemoglobin, Sickle, Humans, In Vitro Techniques, Malaria, Falciparum blood, Middle Aged, Senegal, Antibodies, Protozoan blood, Erythrocytes immunology, Erythrocytes parasitology, Immunoglobulin G blood, Malaria, Falciparum immunology, Malaria, Falciparum parasitology, Plasmodium falciparum immunology
Abstract

To investigate the potential for use of a well-established strain of Plasmodium falciparum as a reference strain for infected red blood cell (IRBC) surface reactivity, we monitored the binding of specific immunoglobulin G (IgG) from immune individuals to the reference Knob-positive FCR3 strain by flow cytometry. To permit interassay comparison for 162 plasma samples drawn after the rainy season, a labeling index (LI) was defined as the percentage of labeled parasites multiplied by the mean peak intensity. An LI ratio (LIR) was then calculated as the LI of the sample divided by the LI of the control. LIRs were calculated for individuals living in Dielmo and Ndiop, two Senegalese villages where P. falciparum is transmitted holoendemically and mesoendemically, respectively. The incidence (persons with an LIR of >3) observed in Dielmo was lower than that observed in Ndiop. Significantly higher LIRs were observed (i) for samples from Ndiop than for samples from Dielmo (P < 0.01) and (ii) in Ndiop, in subjects with hemoglobin AS (HbAS) than in those with hemoglobin AA (P = 0.03). No correlation with the cumulative age-associated immune status of the villagers was evidenced, contrary to antibody (Ab) responses against conserved IRBC-associated antigen (Ag) measured by enzyme-linked immunosorbent assay. These results are consistent with the notions that protection in HbAS individuals may relate to an increased IgG response to IRBC membrane Ags and that cell surface reactivity parallels IgG responses even though it is in itself a distinct indicator of the anti-P. falciparum Ab response. Measures of IgG binding to live IRBC are thus relevant for the functional screening of conserved IRBC-associated Ags that contribute to parasite destruction in vivo, as these Ags might be included in a multitarget vaccine.

Published
2004
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