76 research outputs found

    D’un service à un autre

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    This paper explores health seeking behaviors of pediatric cancer patients in the health system of Mali. The management of pediatric cancer involves the pediatric oncologist, various specialists (pediatric surgeons, anatomopathologists, radiologists) and various hospitals. The paper aims to update the forms of collaboration between the above actors around care. Based on an ethnographic survey, this work lays the foundations for a broader reflection on the organization of paediatric oncology care in Mali. The study sheds light on the child’s cancer care journey by highlighting the determinants of collaboration. It has shown that the management of childhood cancers reveals the socio-economic, professional and geopolitical challenges.Cet article s’intĂ©resse au parcours de soin de l’enfant atteint de cancer dans le systĂšme de santĂ© du Mali. La prise en charge de cette maladie implique, en plus du pĂ©diatre oncologue, diffĂ©rents spĂ©cialistes (chirurgiens pĂ©diatres, anatomopathologistes, radiologues) et sites hospitaliers. Il s’agit ici de mettre Ă  jour les formes de collaboration entre ces diffĂ©rents acteurs autour des soins. À partir d’une enquĂȘte ethnographique, ce travail jette les bases d’une rĂ©flexion plus large sur l’organisation des soins en oncologie pĂ©diatrique au Mali. L’étude a permis d’éclairer le parcours de soin de l’enfant atteint de cancer en mettant en Ă©vidence les facteurs dĂ©terminants de la collaboration. Elle a montrĂ© que la prise en charge des cancers de l’enfant est rĂ©vĂ©latrice des enjeux socioĂ©conomiques, professionnels et gĂ©opolitiques

    PRATIQUES DE CONTROLE DANS LES COLLECTIVITES DECENTRALISEES DU DISTRICT DE BAMAKO

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    Ce papier a pour but principal d’expliquer les pratiques actuelles de contrĂŽle dans les collectivitĂ©s dĂ©centralisĂ©es du District de Bamako. Afin d’aboutir Ă  cet objectif, nous avons posĂ© les questions suivantes : Quelles sont les pratiques actuelles de contrĂŽle dans collectivitĂ©s dĂ©centralisĂ©es du District de Bamako ? Le cadre organique est-il appliquĂ© correctement dans les collectivitĂ©s dĂ©centralisĂ©es du District de Bamako ? Nous avons menĂ© une recherche qualitative pour la confirmation nos propositions. Le guide d’entretien et l’analyse du contenu ont Ă©tĂ© privilĂ©giĂ©s comme technique de recueil des donnĂ©es. Quatorze personnes qui constituent la population mĂšre ont reçu le guide. Seulement cinq (5) personnes ont pu rĂ©pondre. Nous avons adoptĂ© un positionnement interprĂ©tativisme pour analyser les donnĂ©es. Les essentiels rĂ©sultats trouvĂ©s montrent qu’il n’existe pas de plan de formation pour les personnels des collectivitĂ©s dĂ©centralisĂ©es du District de Bamako, donc pas de plan de carriĂšre. Les rĂ©sultats signalent aussi la non implication des responsables de ces diffĂ©rentes communes, l’absence de procĂ©dure, le cumul de fonctions, le manque du personnel compĂ©tent, les malversations financiĂšres et le problĂšme de mobilisation des ressources propres dans les collectivitĂ©s dĂ©centralisĂ©es du District de Bamako. Les rĂ©sultats prĂ©sentent Ă©galement que les collectivitĂ©s dĂ©centralisĂ©es du District de Bamako manquent d’application de cadre organique

    A multi-center, open-label trial to compare the efficacy and pharmacokinetics of Artemether-Lumefantrine in children with severe acute malnutrition versus children without severe acute malnutrition: study protocol for the MAL-NUT study

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    BACKGROUND:Malnutrition and malaria frequently coexist in sub-Saharan African countries. Studies on efficacy of antimalarial treatments usually follow the WHO standardized protocol in which severely malnourished children are systematically excluded.Few studies have assessed the efficacy of chloroquine, sulfadoxine-pyrimethamine and quinine in severe acute malnourished children. Overall, efficacy of these treatments appeared to be reduced, attributed to lower immunity and for some antimalarials altered pharmacokinetic profiles and lower drug concentrations. However, similar research on the efficacy and pharmacokinetic profiles of artemisinin-combination therapies (ACTs) and especially artemether-lumefantrine in malnourished children is currently lacking.The main objective of this study is to assess whether artemether-lumefantrine is less efficacious in children suffering from severe acute malnutrition (SAM) compared to non-SAM children, and if so, to what extent this can be attributed to a sub-optimal pharmacokinetic profile.METHODS/DESIGN:In two sites, Ouelessebougou, Mali and Maradi, Niger, children with uncomplicated microscopically-confirmed P. falciparum malaria aged between 6 and 59 months will be enrolled. Two non-SAM children will be enrolled after the enrolment of each SAM case. Children with severe manifestations of malaria or complications of acute malnutrition needing intensive treatment will be excluded.Treatment intakes will be supervised and children will be followed-up for 42 days, according to WHO guidance for surveillance of antimalarial drug efficacy. Polymerase Chain Reaction genotyping will be used to distinguish recrudescence from re-infection. SAM children will also benefit from the national nutritional rehabilitation program.Outcomes will be compared between the SAM and non-SAM populations. The primary outcome will be adequate clinical and parasitological response at day 28 after PCR correction, estimated by Kaplan-Meier analysis. To assess the pharmacokinetic profile of lumefantrine, a sparse sampling approach will be used with randomized allocation of sampling times (5 per child). A total of 180 SAM children and 360 non-SAM children will be recruited during the 2013 and 2014 malaria seasons.DISCUSSION:This study will provide important information that is currently lacking on the effect of SAM on therapeutic efficacy and pharmacokinetic profile of artemether-lumefantrine. If it shows lower therapeutic efficacy and decreased lumefantrine concentrations, it would inform dose optimization studies in SAM children.TRIAL REGISTRATION:ClinicalTrials.gov: NCT0195890

    Application of Functional Data Analysis to Identify Patterns of Malaria Incidence, to Guide Targeted Control Strategies.

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    We introduce an approach based on functional data analysis to identify patterns of malaria incidence to guide effective targeting of malaria control in a seasonal transmission area. Using functional data method, a smooth function (functional data or curve) was fitted from the time series of observed malaria incidence for each of 575 villages in west-central Senegal from 2008 to 2012. These 575 smooth functions were classified using hierarchical clustering (Ward's method), and several different dissimilarity measures. Validity indices were used to determine the number of distinct temporal patterns of malaria incidence. Epidemiological indicators characterizing the resulting malaria incidence patterns were determined from the velocity and acceleration of their incidences over time. We identified three distinct patterns of malaria incidence: high-, intermediate-, and low-incidence patterns in respectively 2% (12/575), 17% (97/575), and 81% (466/575) of villages. Epidemiological indicators characterizing the fluctuations in malaria incidence showed that seasonal outbreaks started later, and ended earlier, in the low-incidence pattern. Functional data analysis can be used to identify patterns of malaria incidence, by considering their temporal dynamics. Epidemiological indicators derived from their velocities and accelerations, may guide to target control measures according to patterns

    BMJ Open

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    In low-income settings with limited access to diagnosis, COVID-19 information is scarce. In September 2020, after the first COVID-19 wave, Mali reported 3086 confirmed cases and 130 deaths. Most reports originated from Bamako, with 1532 cases and 81 deaths (2.42 million inhabitants). This observed prevalence of 0.06% appeared very low. Our objective was to estimate SARS-CoV-2 infection among inhabitants of Bamako, after the first epidemic wave. We assessed demographic, social and living conditions, health behaviours and knowledges associated with SARS-CoV-2 seropositivity. We conducted a cross-sectional multistage household survey during September 2020, in three neighbourhoods of the commune VI (Bamako), where 30% of the cases were reported. We recruited 1526 inhabitants in 3 areas, that is, 306 households, and 1327 serological results (≄1 years), 220 household questionnaires and collected answers for 962 participants (≄12 years). We measured serological status, detecting SARS-CoV-2 spike protein antibodies in blood sampled. We documented housing conditions and individual health behaviours through questionnaires among participants. We estimated the number of SARS-CoV-2 infections and deaths in the population of Bamako using the age and sex distributions. The prevalence of SARS-CoV-2 seropositivity was 16.4% (95% CI 15.1% to 19.1%) after adjusting on the population structure. This suggested that ~400 000 cases and ~2000 deaths could have occurred of which only 0.4% of cases and 5% of deaths were officially reported. Questionnaires analyses suggested strong agreement with washing hands but lower acceptability of movement restrictions (lockdown/curfew), and mask wearing. The first wave of SARS-CoV-2 spread broadly in Bamako. Expected fatalities remained limited largely due to the population age structure and the low prevalence of comorbidities. Improving diagnostic capacities to encourage testing and preventive behaviours, and avoiding the spread of false information remain key pillars, regardless of the developed or developing setting. This study was registered in the registry of the ethics committee of the Faculty of Medicine and Odonto-Stomatology and the Faculty of Pharmacy, Bamako, Mali, under the number: 2020/162/CA/FMOS/FAPH

    Plasmodium falciparum clearance with artemisinin-based combination therapy (ACT) in patients with glucose-6-phosphate dehydrogenase deficiency in Mali

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    URL : http://www.malariajournal.com/content/9/1/332Background: Artemisinin-based combination therapy (ACT) is currently the most effective medicine for the treatment of uncomplicated malaria. Artemisinin has previously been shown to increase the clearance of Plasmodium falciparum in malaria patients with haemoglobin E trait, but it did not increase parasite inhibition in an in vitro study using haemoglobin AS erythrocytes. The current study describes the efficacy of artemisinin derivatives on P. falciparum clearance in patients with glucose-6-phosphate dehydrogenase deficiency (G6PD), a haemoglobin enzyme deficiency, not yet studied in the same context, but nonetheless is a common in malaria endemic areas, associated with host protection against uncomplicated and severe malaria. The impact of G6PD deficiency on parasite clearance with ACT treatment was compared between G6PD-deficient patients and G6PD-normal group. Methods: Blood samples from children and adults participants (1 to 70 years old) with uncomplicated P. falciparum malaria residing in Kambila, Mali were analysed. Study participants were randomly assigned to receive either artemether-lumefantrine (Coartem¼) or artesunate plus mefloquine (Artequinℱ). A restriction-fragment length polymorphism analysis of PCR-amplified DNA samples was used to identify the (A-) allele of the gene mutation responsible for G6PD deficiency (G6PD*A-). 470 blood samples were thus analysed and of these, DNA was extracted from 315 samples using the QIAamp kit for PCR to identify the G6PD*A- gene. Results

    Plasmodium falciparum transcription in different clinical presentations of malaria associates with circulation time of infected erythrocytes

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    Following Plasmodium falciparum infection, individuals can remain asymptomatic, present with mild fever in uncomplicated malaria cases, or show one or more severe malaria symptoms. Several studies have investigated associations between parasite transcription and clinical severity, but no broad conclusions have yet been drawn. Here, we apply a series of bioinformatic approaches based on P. falciparum’s tightly regulated transcriptional pattern during its ~48-hour intraerythrocytic developmental cycle (IDC) to publicly available transcriptomes of parasites obtained from malaria cases of differing clinical severity across multiple studies. Our analysis shows that within each IDC, the circulation time of infected erythrocytes without sequestering to endothelial cells decreases with increasing parasitaemia or disease severity. Accordingly, we find that the size of circulating infected erythrocytes is inversely related to parasite density and disease severity. We propose that enhanced dhesiveness of infected erythrocytes leads to a rapid increase in parasite burden, promoting higher parasitaemia and increased disease severity
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