Your search keyword '"Djimdé, A"' showing total 15 results

1. Genome-wide association study of leprosy in Malawi and Mali.

Author

James J Gilchrist, Kathryn Auckland, Tom Parks, Alexander J Mentzer, Lily Goldblatt, Vivek Naranbhai, Gavin Band, Kirk A Rockett, Ousmane B Toure, Salimata Konate, Sibiri Sissoko, Abdoulaye A Djimdé, Mahamadou A Thera, Ogobara K Doumbo, Samba Sow, Sian Floyd, Jörg M Pönnighaus, David K Warndorff, Amelia C Crampin, Paul E M Fine, Benjamin P Fairfax, and Adrian V S Hill

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

Leprosy is a chronic infection of the skin and peripheral nerves caused by Mycobacterium leprae. Despite recent improvements in disease control, leprosy remains an important cause of infectious disability globally. Large-scale genetic association studies in Chinese, Vietnamese and Indian populations have identified over 30 susceptibility loci for leprosy. There is a significant burden of leprosy in Africa, however it is uncertain whether the findings of published genetic association studies are generalizable to African populations. To address this, we conducted a genome-wide association study (GWAS) of leprosy in Malawian (327 cases, 436 controls) and Malian (247 cases, 368 controls) individuals. In that analysis, we replicated four risk loci previously reported in China, Vietnam and India; MHC Class I and II, LACC1 and SLC29A3. We further identified a novel leprosy susceptibility locus at 10q24 (rs2015583; combined p = 8.81 × 10-9; OR = 0.51 [95% CI 0.40 - 0.64]). Using publicly-available data we characterise regulatory activity at this locus, identifying ACTR1A as a candidate mediator of leprosy risk. This locus shows evidence of recent positive selection and demonstrates pleiotropy with established risk loci for inflammatory bowel disease and childhood-onset asthma. A shared genetic architecture for leprosy and inflammatory bowel disease has been previously described. We expand on this, strengthening the hypothesis that selection pressure driven by leprosy has shaped the evolution of autoimmune and atopic disease in modern populations. More broadly, our data highlights the importance of defining the genetic architecture of disease across genetically diverse populations, and that disease insights derived from GWAS in one population may not translate to all affected populations.

Published

2022

2. The cardiovascular effects of amodiaquine and structurally related antimalarials: An individual patient data meta-analysis.

Author

Xin Hui S Chan, Ilsa L Haeusler, Yan Naung Win, James Pike, Borimas Hanboonkunupakarn, Maryam Hanafiah, Sue J Lee, Abdoulaye Djimdé, Caterina I Fanello, Jean-René Kiechel, Marcus Vg Lacerda, Bernhards Ogutu, Marie A Onyamboko, André M Siqueira, Elizabeth A Ashley, Walter Rj Taylor, and Nicholas J White

Subjects

Medicine

Abstract

BackgroundAmodiaquine is a 4-aminoquinoline antimalarial similar to chloroquine that is used extensively for the treatment and prevention of malaria. Data on the cardiovascular effects of amodiaquine are scarce, although transient effects on cardiac electrophysiology (electrocardiographic QT interval prolongation and sinus bradycardia) have been observed. We conducted an individual patient data meta-analysis to characterise the cardiovascular effects of amodiaquine and thereby support development of risk minimisation measures to improve the safety of this important antimalarial.Methods and findingsStudies of amodiaquine for the treatment or prevention of malaria were identified from a systematic review. Heart rates and QT intervals with study-specific heart rate correction (QTcS) were compared within studies and individual patient data pooled for multivariable linear mixed effects regression. The meta-analysis included 2,681 patients from 4 randomised controlled trials evaluating artemisinin-based combination therapies (ACTs) containing amodiaquine (n = 725), lumefantrine (n = 499), piperaquine (n = 716), and pyronaridine (n = 566), as well as monotherapy with chloroquine (n = 175) for uncomplicated malaria. Amodiaquine prolonged QTcS (mean = 16.9 ms, 95% CI: 15.0 to 18.8) less than chloroquine (21.9 ms, 18.3 to 25.6, p = 0.0069) and piperaquine (19.2 ms, 15.8 to 20.5, p = 0.0495), but more than lumefantrine (5.6 ms, 2.9 to 8.2, p < 0.001) and pyronaridine (-1.2 ms, -3.6 to +1.3, p < 0.001). In individuals aged ≥12 years, amodiaquine reduced heart rate (mean reduction = 15.2 beats per minute [bpm], 95% CI: 13.4 to 17.0) more than piperaquine (10.5 bpm, 7.7 to 13.3, p = 0.0013), lumefantrine (9.3 bpm, 6.4 to 12.2, p < 0.001), pyronaridine (6.6 bpm, 4.0 to 9.3, p < 0.001), and chloroquine (5.9 bpm, 3.2 to 8.5, p < 0.001) and was associated with a higher risk of potentially symptomatic sinus bradycardia (≤50 bpm) than lumefantrine (risk difference: 14.8%, 95% CI: 5.4 to 24.3, p = 0.0021) and chloroquine (risk difference: 8.0%, 95% CI: 4.0 to 12.0, p < 0.001). The effect of amodiaquine on the heart rate of children aged ConclusionsWhile caution is advised in the use of amodiaquine in patients aged ≥12 years with concomitant use of heart rate-reducing medications, serious cardiac conduction disorders, or risk factors for torsade de pointes, there have been no serious cardiovascular events reported after amodiaquine in widespread use over 7 decades. Amodiaquine and structurally related antimalarials in the World Health Organization (WHO)-recommended dose regimens alone or in ACTs are safe for the treatment and prevention of malaria.

Published

2021

3. Genome-wide association study of leprosy in Malawi and Mali

Author

Gilchrist, James J., primary, Auckland, Kathryn, additional, Parks, Tom, additional, Mentzer, Alexander J., additional, Goldblatt, Lily, additional, Naranbhai, Vivek, additional, Band, Gavin, additional, Rockett, Kirk A., additional, Toure, Ousmane B., additional, Konate, Salimata, additional, Sissoko, Sibiri, additional, Djimdé, Abdoulaye A., additional, Thera, Mahamadou A., additional, Doumbo, Ogobara K., additional, Sow, Samba, additional, Floyd, Sian, additional, Pönnighaus, Jörg M., additional, Warndorff, David K., additional, Crampin, Amelia C., additional, Fine, Paul E. M., additional, Fairfax, Benjamin P., additional, and Hill, Adrian V. S., additional

Published

2022

4. Dermatophytosis among Schoolchildren in Three Eco-climatic Zones of Mali.

Author

Oumar Coulibaly, Abdoulaye K Kone, Safiatou Niaré-Doumbo, Siaka Goïta, Jean Gaudart, Abdoulaye A Djimdé, Renaud Piarroux, Ogobara K Doumbo, Mahamadou A Thera, and Stéphane Ranque

Subjects

Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270

Abstract

Dermatophytosis, and particularly the subtype tinea capitis, is common among African children; however, the risk factors associated with this condition are poorly understood. To describe the epidemiology of dermatophytosis in distinct eco-climatic zones, three cross-sectional surveys were conducted in public primary schools located in the Sahelian, Sudanian and Sudano-Guinean eco-climatic zones in Mali.Among 590 children (average age 9.7 years) the overall clinical prevalence of tinea capitis was 39.3%. Tinea capitis prevalence was 59.5% in the Sudano-Guinean zone, 41.6% in the Sudanian zone and 17% in the Sahelian eco-climatic zone. Microsporum audouinii was isolated primarily from large and/or microsporic lesions. Trichophyton soudanense was primarily isolated from trichophytic lesions. Based on the multivariate analysis, tinea capitis was independently associated with male gender (OR = 2.51, 95%CI [1.74-3.61], P

Published

2016

5. Tools and Strategies for Malaria Control and Elimination: What Do We Need to Achieve a Grand Convergence in Malaria?

Author

Janet Hemingway, Rima Shretta, Timothy N C Wells, David Bell, Abdoulaye A Djimdé, Nicole Achee, and Gao Qi

Subjects

Biology (General), QH301-705.5

Abstract

Progress made in malaria control during the past decade has prompted increasing global dialogue on malaria elimination and eradication. The product development pipeline for malaria has never been stronger, with promising new tools to detect, treat, and prevent malaria, including innovative diagnostics, medicines, vaccines, vector control products, and improved mechanisms for surveillance and response. There are at least 25 projects in the global malaria vaccine pipeline, as well as 47 medicines and 13 vector control products. In addition, there are several next-generation diagnostic tools and reference methods currently in development, with many expected to be introduced in the next decade. The development and adoption of these tools, bolstered by strategies that ensure rapid uptake in target populations, intensified mechanisms for information management, surveillance, and response, and continued financial and political commitment are all essential to achieving global eradication.

Published

2016

6. A Non-Inferiority, Individually Randomized Trial of Intermittent Screening and Treatment versus Intermittent Preventive Treatment in the Control of Malaria in Pregnancy.

Author

Harry Tagbor, Matthew Cairns, Kalifa Bojang, Sheick Oumar Coulibaly, Kassoum Kayentao, John Williams, Ismaela Abubakar, Francis Akor, Khalifa Mohammed, Richard Bationo, Edgar Dabira, Alamissa Soulama, Moussa Djimdé, Etienne Guirou, Timothy Awine, Stephen Quaye, Fanta Njie, Jaume Ordi, Ogobara Doumbo, Abraham Hodgson, Abraham Oduro, Steven Meshnick, Steve Taylor, Pascal Magnussen, Feiko ter Kuile, Arouna Woukeu, Paul Milligan, Daniel Chandramohan, and Brian Greenwood

Subjects

Medicine, Science

Abstract

BACKGROUND:The efficacy of intermittent preventive treatment for malaria with sulfadoxine-pyrimethamine (IPTp-SP) in pregnancy is threatened in parts of Africa by the emergence and spread of resistance to SP. Intermittent screening with a rapid diagnostic test (RDT) and treatment of positive women (ISTp) is an alternative approach. METHODS AND FINDINGS:An open, individually randomized, non-inferiority trial of IPTp-SP versus ISTp was conducted in 5,354 primi- or secundigravidae in four West African countries with a low prevalence of resistance to SP (The Gambia, Mali, Burkina Faso and Ghana). Women in the IPTp-SP group received SP on two or three occasions whilst women in the ISTp group were screened two or three times with a RDT and treated if positive for malaria with artemether-lumefantrine (AL). ISTp-AL was non-inferior to IPTp-SP in preventing low birth weight (LBW), anemia and placental malaria, the primary trial endpoints. The prevalence of LBW was 15.1% and 15.6% in the IPTp-SP and ISTp-AL groups respectively (OR = 1.03 [95% CI: 0.88, 1.22]). The mean hemoglobin concentration at the last clinic attendance before delivery was 10.97g/dL and 10.94g/dL in the IPTp-SP and ISTp-AL groups respectively (mean difference: -0.03 g/dL [95% CI: -0.13, +0.06]). Active malaria infection of the placenta was found in 24.5% and in 24.2% of women in the IPTp-SP and ISTp-AL groups respectively (OR = 0.95 [95% CI 0.81, 1.12]). More women in the ISTp-AL than in the IPTp-SP group presented with malaria parasitemia between routine antenatal clinics (310 vs 182 episodes, rate difference: 49.4 per 1,000 pregnancies [95% CI 30.5, 68.3], but the number of hospital admissions for malaria was similar in the two groups. CONCLUSIONS:Despite low levels of resistance to SP in the study areas, ISTp-AL performed as well as IPTp-SP. In the absence of an effective alternative medication to SP for IPTp, ISTp-AL is a potential alternative to IPTp in areas where SP resistance is high. It may also have a role in areas where malaria transmission is low and for the prevention of malaria in HIV positive women receiving cotrimoxazole prophylaxis in whom SP is contraindicated. TRIAL REGISTRATION:ClinicalTrials.gov NCT01084213 Pan African Clinical trials Registry PACT201202000272122.

Published

2015

7. The cardiovascular effects of amodiaquine and structurally related antimalarials: An individual patient data meta-analysis

Author

Chan, Xin Hui S., primary, Haeusler, Ilsa L., additional, Win, Yan Naung, additional, Pike, James, additional, Hanboonkunupakarn, Borimas, additional, Hanafiah, Maryam, additional, Lee, Sue J., additional, Djimdé, Abdoulaye, additional, Fanello, Caterina I., additional, Kiechel, Jean-René, additional, Lacerda, Marcus VG, additional, Ogutu, Bernhards, additional, Onyamboko, Marie A., additional, Siqueira, André M., additional, Ashley, Elizabeth A., additional, Taylor, Walter RJ, additional, and White, Nicholas J., additional

Published

2021

8. Surveillance of travellers: an additional tool for tracking antimalarial drug resistance in endemic countries.

Author

Myriam Gharbi, Jennifer A Flegg, Bruno Pradines, Ako Berenger, Magatte Ndiaye, Abdoulaye A Djimdé, Cally Roper, Véronique Hubert, Eric Kendjo, Meera Venkatesan, Philippe Brasseur, Oumar Gaye, André T Offianan, Louis Penali, Jacques Le Bras, Philippe J Guérin, and Members of the French National Reference Center for Imported Malaria Study

Subjects

Medicine, Science

Abstract

IntroductionThere are growing concerns about the emergence of resistance to artemisinin-based combination therapies (ACTs). Since the widespread adoption of ACTs, there has been a decrease in the systematic surveillance of antimalarial drug resistance in many malaria-endemic countries. The aim of this work was to test whether data on travellers returning from Africa with malaria could serve as an additional surveillance system of local information sources for the emergence of drug resistance in endemic-countries.MethodologyData were collected from travellers with symptomatic Plasmodium falciparum malaria returning from Senegal (n = 1,993), Mali (n = 2,372), Cote d'Ivoire (n = 4,778) or Cameroon (n = 3,272) and recorded in the French Malaria Reference Centre during the period 1996-2011. Temporal trends of the proportion of parasite isolates that carried the mutant genotype, pfcrt 76T, a marker of resistance to chloroquine (CQ) and pfdhfr 108N, a marker of resistance to pyrimethamine, were compared for travellers and within-country surveys that were identified through a literature review in PubMed. The in vitro response to CQ was also compared between these two groups for parasites from Senegal.ResultsThe trends in the proportion of parasites that carried pfcrt 76T, and pfdhfr 108N, were compared for parasites from travellers and patients within-country using the slopes of the curves over time; no significant differences in the trends were found for any of the 4 countries. These results were supported by in vitro analysis of parasites from the field in Senegal and travellers returning to France, where the trends were also not significantly different.ConclusionThe results have not shown different trends in resistance between parasites derived from travellers or from parasites within-country. This work highlights the value of an international database of drug responses in travellers as an additional tool to assess the emergence of drug resistance in endemic areas where information is limited.

Published

2013

9. First detection of Leishmania major DNA in Sergentomyia (Spelaeomyia) darlingi from cutaneous leishmaniasis foci in Mali.

Author

Zohra Berdjane-Brouk, Abdoulaye K Koné, Abdoulaye A Djimdé, Rémi N Charrel, Christophe Ravel, Pascal Delaunay, Pascal del Giudice, Adama Z Diarra, Siala Doumbo, Siaka Goita, Mahamadou A Thera, Jérôme Depaquit, Pierre Marty, Ogobara K Doumbo, and Arezki Izri

Subjects

Medicine, Science

Abstract

BackgroundLeishmania major complex is the main causative agent of zoonotic cutaneous leishmaniasis (ZCL) in the Old World. Phlebotomus papatasi and Phlebotomus duboscqi are recognized vectors of L. major complex in Northern and Southern Sahara, respectively. In Mali, ZCL due to L. major is an emerging public health problem, with several cases reported from different parts of the country. The main objective of the present study was to identify the vectors of Leishmania major in the Bandiagara area, in Mali.Methodology/principal findingsAn entomological survey was carried out in the ZCL foci of Bandiagara area. Sandflies were collected using CDC miniature light traps and sticky papers. In the field, live female Phlebotomine sandflies were identified and examined for the presence of promastigotes. The remaining sandflies were identified morphologically and tested for Leishmania by PCR in the ITS2 gene. The source of blood meal of the engorged females was determined using the cyt-b sequence. Out of the 3,259 collected sandflies, 1,324 were identified morphologically, and consisted of 20 species, of which four belonged to the genus Phlebotomus and 16 to the genus Sergentomyia. Leishmania major DNA was detected by PCR in 7 of the 446 females (1.6%), specifically 2 out of 115 Phlebotomus duboscqi specimens, and 5 from 198 Sergentomyia darlingi specimens. Human DNA was detected in one blood-fed female S. darlingi positive for L. major DNA.ConclusionOur data suggest the possible involvement of P. duboscqi and potentially S. darlingi in the transmission of ZCL in Mali.

Published

2012

10. Design of group IIA secreted/synovial phospholipase A(2) inhibitors: an oxadiazolone derivative suppresses chondrocyte prostaglandin E(2) secretion.

Author

Jean-Edouard Ombetta, Natacha Thelier, Chang Zhi Dong, Stéphanie Plocki, Lydia Tsagris, François Rannou, France Massicot, Atimé Djimdé, Elissar El-Hayek, Yiming Shi, Françoise Heymans, Nohad Gresh, and Caroline Chauvet

Subjects

Medicine, Science

Abstract

Group IIA secreted/synovial phospholipase A(2) (GIIAPLA(2)) is an enzyme involved in the synthesis of eicosanoids such as prostaglandin E(2) (PGE(2)), the main eicosanoid contributing to pain and inflammation in rheumatic diseases. We designed, by molecular modeling, 7 novel analogs of 3-{4-[5(indol-1-yl)pentoxy]benzyl}-4H-1,2,4-oxadiazol-5-one, denoted C1, an inhibitor of the GIIAPLA(2) enzyme. We report the results of molecular dynamics studies of the complexes between these derivatives and GIIAPLA(2), along with their chemical synthesis and results from PLA(2) inhibition tests. Modeling predicted some derivatives to display greater GIIAPLA(2) affinities than did C1, and such predictions were confirmed by in vitro PLA(2) enzymatic tests. Compound C8, endowed with the most favorable energy balance, was shown experimentally to be the strongest GIIAPLA(2) inhibitor. Moreover, it displayed an anti-inflammatory activity on rabbit articular chondrocytes, as shown by its capacity to inhibit IL-1beta-stimulated PGE(2) secretion in these cells. Interestingly, it did not modify the COX-1 to COX-2 ratio. C8 is therefore a potential candidate for anti-inflammatory therapy in joints.

Published

2010

11. Dermatophytosis among Schoolchildren in Three Eco-climatic Zones of Mali

Author

Coulibaly, Oumar, primary, Kone, Abdoulaye K., additional, Niaré-Doumbo, Safiatou, additional, Goïta, Siaka, additional, Gaudart, Jean, additional, Djimdé, Abdoulaye A., additional, Piarroux, Renaud, additional, Doumbo, Ogobara K., additional, Thera, Mahamadou A., additional, and Ranque, Stéphane, additional

Published

2016

12. Tools and Strategies for Malaria Control and Elimination: What Do We Need to Achieve a Grand Convergence in Malaria?

Author

Hemingway, Janet, primary, Shretta, Rima, additional, Wells, Timothy N. C., additional, Bell, David, additional, Djimdé, Abdoulaye A., additional, Achee, Nicole, additional, and Qi, Gao, additional

Published

2016

13. A Non-Inferiority, Individually Randomized Trial of Intermittent Screening and Treatment versus Intermittent Preventive Treatment in the Control of Malaria in Pregnancy

Author

Tagbor, Harry, primary, Cairns, Matthew, additional, Bojang, Kalifa, additional, Coulibaly, Sheick Oumar, additional, Kayentao, Kassoum, additional, Williams, John, additional, Abubakar, Ismaela, additional, Akor, Francis, additional, Mohammed, Khalifa, additional, Bationo, Richard, additional, Dabira, Edgar, additional, Soulama, Alamissa, additional, Djimdé, Moussa, additional, Guirou, Etienne, additional, Awine, Timothy, additional, Quaye, Stephen, additional, Njie, Fanta, additional, Ordi, Jaume, additional, Doumbo, Ogobara, additional, Hodgson, Abraham, additional, Oduro, Abraham, additional, Meshnick, Steven, additional, Taylor, Steve, additional, Magnussen, Pascal, additional, ter Kuile, Feiko, additional, Woukeu, Arouna, additional, Milligan, Paul, additional, Chandramohan, Daniel, additional, and Greenwood, Brian, additional

Published

2015

14. First Detection of Leishmania major DNA in Sergentomyia (Spelaeomyia) darlingi from Cutaneous Leishmaniasis Foci in Mali

Author

Berdjane-Brouk, Zohra, primary, Koné, Abdoulaye K., additional, Djimdé, Abdoulaye A., additional, Charrel, Rémi N., additional, Ravel, Christophe, additional, Delaunay, Pascal, additional, del Giudice, Pascal, additional, Diarra, Adama Z., additional, Doumbo, Siala, additional, Goita, Siaka, additional, Thera, Mahamadou A., additional, Depaquit, Jérôme, additional, Marty, Pierre, additional, Doumbo, Ogobara K., additional, and Izri, Arezki, additional

Published

2012

15. Design of Group IIA Secreted/Synovial Phospholipase A2 Inhibitors: An Oxadiazolone Derivative Suppresses Chondrocyte Prostaglandin E2 Secretion

Author

Ombetta, Jean-Edouard, primary, Thelier, Natacha, additional, Dong, Chang Zhi, additional, Plocki, Stéphanie, additional, Tsagris, Lydia, additional, Rannou, François, additional, Massicot, France, additional, Djimdé, Atimé, additional, El-Hayek, Elissar, additional, Shi, Yiming, additional, Heymans, Françoise, additional, Gresh, Nohad, additional, and Chauvet, Caroline, additional

Published

2010