Your search keyword '"Diawara, Silman"' showing total 11 results

1. Ex vivo activity of Proveblue, a methylene blue, against field isolates of Plasmodium falciparum in Dakar, Senegal from 2013–2015

Author

Fall, Bécaye, Madamet, Marylin, Diawara, Silman, Briolant, Sébastien, Wade, Khalifa Ababacar, Lo, Gora, Nakoulima, Aminata, Fall, Mansour, Bercion, Raymond, Kounta, Mame Bou, Amalvict, Rémi, Benoit, Nicolas, Gueye, Mamadou Wague, Diatta, Bakary, Wade, Boubacar, and Pradines, Bruno

Published

2017

2. Absence of association between polymorphisms in the K13 gene and the presence of Plasmodium falciparum parasites at day 3 after treatment with artemisinin derivatives in Senegal

Author

Madamet, Marylin, Kounta, Mame Bou, Wade, Khalifa Ababacar, Lo, Gora, Diawara, Silman, Fall, Mansour, Bercion, Raymond, Nakoulima, Aminata, Fall, Khadidiatou Ba, Benoit, Nicolas, Gueye, Mamadou Wague, Fall, Bécaye, Diatta, Bakary, and Pradines, Bruno

Published

2017

3. Low polymorphisms in pfact, pfugt and pfcarl genes in African Plasmodium falciparum isolates and absence of association with susceptibility to common anti-malarial drugs

Author

Foguim, Francis Tsombeng, Robert, Marie Gladys, Gueye, Mamadou Wagué, Gendrot, Mathieu, Diawara, Silman, Mosnier, Joel, Amalvict, Rémy, Benoit, Nicolas, Bercion, Raymond, Fall, Bécaye, Madamet, Marylin, Pradines, Bruno, and The French National Reference Centre for Imported Malaria Study Group

Published

2019

4. Confirmation of Plasmodium falciparum in vitro resistance to monodesethylamodiaquine and chloroquine in Dakar, Senegal, in 2015.

Author

Diawara, Silman, Madamet, Marylin, Kounta, Mame Bou, Lo, Gora, Wade, Khalifa Ababacar, Nakoulima, Aminata, Bercion, Raymond, Amalvict, Rémy, Gueye, Mamadou Wague, Fall, Bécaye, Diatta, Bakary, and Pradines, Bruno

Subjects

*ANTIMALARIALS, *PLASMODIUM falciparum, *ARTEMISININ, *CHLOROQUINE, *SOCIAL history

Abstract

Background: In response to increasing resistance to anti-malarial drugs, Senegal adopted artemisinin-based combination therapy (ACT) as the first-line treatment for uncomplicated malaria in 2006. However, resistance of Plasmodium falciparum parasites to artemisinin derivatives, characterized by delayed parasite clearance after treatment with ACT or artesunate monotherapy, has recently emerged and rapidly spread in Southeast Asia. After 10 years of stability with rates ranging from 5.6 to 11.8%, the prevalence of parasites with reduced susceptibility in vitro to monodesethylamodiaquine, the active metabolite of an ACT partner drug, increased to 30.6% in 2014 in Dakar. Additionally, after a decrease of the in vitro chloroquine resistance in Dakar in 2009-2011, the prevalence of parasites that showed in vitro chloroquine resistance increased again to approximately 50% in Dakar since 2013. The aim of this study was to follow the evolution of the susceptibility to ACT partners and other anti-malarial drugs in 2015 in Dakar. An in vitro test is the only method currently available to provide an early indication of resistance to ACT partners. Results: Thirty-two P. falciparum isolates collected in 2015 in Dakar were analysed using a standard ex vivo assay based on an HRP2 ELISA. The prevalence of P. falciparum parasites with reduced susceptibility in vitro to monodesethylamodiaquine, chloroquine, mefloquine, doxycycline and quinine was 28.1, 46.9, 45.2, 31.2 and 9.7%, respectively. None of the parasites were resistant to lumefantrine, piperaquine, pyronaridine, dihydroartemisinin and artesunate. These results confirm an increase in the reduced susceptibility to monodesethylamodiaquine observed in 2014 in Dakar and the chloroquine resistance observed in 2013. The in vitro resistance seems to be established in Dakar. Additionally, the prevalence of parasites with reduced susceptibility to doxycycline has increased two-fold compared to 2014. Conclusions: The establishment of a reduced susceptibility to monodesethylamodiaquine as well as chloroquine resistance, and the emergence of a reduced susceptibility to doxycycline are disturbing. The in vitro and in vivo surveillance of anti-malarial drugs must be implemented in Senegal. [ABSTRACT FROM AUTHOR]

Published

2017

5. High-quality draft genome sequence and description of Haemophilus massiliensis sp. nov.

Author

Lo, Cheikh Ibrahima, Sankar, Senthil Alias, Fall, Bécaye, Sambe-Ba, Bissoume, Diawara, Silman, Gueye, Mamadou Wague, Mediannikov, Oleg, Blanc-Tailleur, Caroline, Wade, Boubacar, Raoult, Didier, Fournier, Pierre-Edouard, and Fenollar, Florence

Subjects

HAEMOPHILUS, NUCLEOTIDE sequencing, ASCITIC fluids, RIBOSOMAL RNA, PASTEURELLACEAE, MATRIX-assisted laser desorption-ionization, WOMEN patients

Abstract

Strain FF7T was isolated from the peritoneal fluid of a 44-year-old woman who suffered from pelvic peritonitis. This strain exhibited a 16S rRNA sequence similarity of 94.8% 16S rRNA sequence identity with Haemophilus parasuis, the phylogenetically closest species with a name with standing in nomenclature and a poor MALDI-TOF MS score (1.32 to 1.56) that does not allow any reliable identification. Using a polyphasic study made of phenotypic and genomic analyses, strain FF7T was a Gram-negative, facultatively anaerobic rod and member of the family Pasteurellaceae. It exhibited a genome of 2,442,548 bp long genome (one chromosome but no plasmid) contains 2,319 protein-coding and 67 RNA genes, including 6 rRNA operons. On the basis of these data, we propose the creation of Haemophilus massiliensis sp. nov. with strain FF7T (= CSUR P859 = DSM 28247) as the type strain. [ABSTRACT FROM AUTHOR]

Published

2016

6. MALDI-TOF Mass Spectrometry: A Powerful Tool for Clinical Microbiology at Hôpital Principal de Dakar, Senegal (West Africa).

Author

Lo, Cheikh I., Fall, Bécaye, Sambe-Ba, Bissoume, Diawara, Silman, Gueye, Mamadou W., Mediannikov, Oleg, Sokhna, Cheikh, Faye, Ngor, Diemé, Yaya, Wade, Boubacar, Raoult, Didier, and Fenollar, Florence

Subjects

MEDICAL microbiology, MATRIX-assisted laser desorption-ionization, TIME-of-flight mass spectrometry, ACHROMOBACTER

Abstract

Our team in Europe has developed the routine clinical laboratory identification of microorganisms by matrix-assisted laser desorption ionization time-of-flight (MALDI-TOF) mass spectrometry (MS). To evaluate the utility of MALDI-TOF MS in tropical Africa in collaboration with local teams, we installed an apparatus in the Hôpital Principal de Dakar (Senegal), performed routine identification of isolates, and confirmed or completed their identification in France. In the case of discordance or a lack of identification, molecular biology was performed. Overall, 153/191 (80.1%) and 174/191 (91.1%) isolates yielded an accurate and concordant identification for the species and genus, respectively, with the 2 different MALDI-TOF MSs in Dakar and Marseille. The 10 most common bacteria, representing 94.2% of all bacteria routinely identified in the laboratory in Dakar (Escherichia coli, Klebsiella pneumoniae, Streptococcus agalactiae, Acinetobacter baumannii, Pseudomonas aeruginosa, Staphylococcus aureus, Staphylococcus haemolyticus, Enterobacter cloacae, Enterococcus faecalis, and Staphylococcus epidermidis) were accurately identified with the MALDI-TOF MS in Dakar. The most frequent misidentification in Dakar was at the species level for Achromobacter xylosoxidans, which was inaccurately identified as Achromobacter denitrificans, and the bacteria absent from the database, such as Exiguobacterium aurientacum or Kytococcus schroeteri, could not be identified. A difficulties were observed with MALDI-TOF MS for Bacillus sp. or oral streptococci. 16S rRNA sequencing identified a novel bacterium, “Necropsobacter massiliensis.” The robust identification of microorganisms by MALDI-TOF MS in Dakar and Marseille demonstrates that MALDI-TOF MS can be used as a first-line tool in clinical microbiology laboratories in tropical countries. [ABSTRACT FROM AUTHOR]

Published

2015

7. Low prevalences of HIV infection and HSV genital shedding in the general adult female population in Senegal.

Author

Diawara, Silman, Bélec, Laurent, Dem, Ahmadou, Mbaye, Seydou, Ndiaye, Halimatou Diop, Matta, Mathieu, Gueye, Sokhna Bousso, Mboup, Souleymane, and Kane, Coumba Toure

Subjects

*GENITALIA infections, *DISEASE prevalence, *HIV infections, *HERPES simplex virus, *SECRETION, *SOCIODEMOGRAPHIC factors

Abstract

Introduction: Herpes simplex virus (HSV) is the main co-factor for heterosexual transmission of the human immunodeficiency virus (HIV) in sub-Saharan Africa, and could be involved in the dynamics of the HIV epidemic in Senegal. Methodology: Genital shedding of HSV was evaluated in adult females who had visited the provincial healthcare centres in Diass, Louga, and Kebemer in Senegal. Study subjects were interviewed by a healthcare worker for sociodemographic characteristics and sexual behavior, and HIV serology was offered. In addition, cervical secretion lavage samples were evaluated for HSV DNA by real-time polymerase chain reaction (PCR), the melting curve analysis of which permitted distinction between HSV type 1 (HSV-1) and HSV type 2 (HSV-2). Results: Among 302 women (mean age, 40 years) enrolled, none were infected by HIV. The mean age at first sexual intercourse was 20 years, and the mean number of sexual partners in the previous year was 1.3 (range, 1-7). Only 6 of 302 (1.9%) women had cervico-vaginal secretions positive for HSV DNA. No association between HSV DNA shedding and any sociodemographic or biological variables was found. Surprisingly, genital shedding of HSV-1 was found in two (0.7%) women, representing 33% of herpes-shedding women, and HSV-2 in four (1.5%) women. Conclusions: Taken together, our observations indicate a low prevalence of HSV DNA genital shedding in adult Senegalese women. [ABSTRACT FROM AUTHOR]

Published

2015

8. The Ongoing Revolution of MALDI-TOF Mass Spectrometry for Microbiology Reaches Tropical Africa.

Author

Fall, Bécaye, Lo, Cheikh Ibrahima, Samb-Ba, Bissoume, Perrot, Nadine, Diawara, Silman, Gueye, Mamadou Wague, Sow, Kowry, Aubadie-Ladrix, Maxence, Mediannikov, Oleg, Sokhna, Cheikh, Diemé, Yaya, Chatellier, Sonia, Wade, Boubacar, Raoult, Didier, and Fenollar, Florence

Published

2015

9. Low seroprevalence of herpes simplex virus type 2 among pregnant women in Senegal.

Author

Diawara, Silman, Kane, Coumba Toure, Legoff, Jérôme, Gaye, Astou Gueye, Mboup, Souleymane, and Bélec, Laurent

Subjects

HERPES simplex virus, HIV-positive women, HERPESVIRUS diseases, HIV infections, PREGNANT women, SKIN infections, PREGNANCY, SEXUALLY transmitted diseases, MOTHERHOOD

Abstract

Herpes simplex virus type 2 (HSV-2) is considered as a major co-factor of both sexual transmission and acquisition of the human immunodeficiency virus (HIV). The HIV epidemic in Senegal is characterized by a remarkable and stable low prevalence. Whether HSV-2 may also constitute a possible co-factor favouring the spreading of HIV epidemic in Senegal is yet unknown. This prompted us to evaluate the HSV-2 seroprevalence in the sentinel population of pregnant women in Senegal. Two hundred and sixty pregnant women attending Roi Baudouin maternity in the capital city Dakar (n = 14; 135) and the antenatal clinic in Kaolack (n = 125), the third city of Senegal, were prospectively recruited between March and August 2003. Fifty-six women (22%) were positive for HSV-2 serology. The prevalence of HSV-2 seropositivity was higher in women living in Dakar (26%) than in those living in Kaolack (16%) (P < 0.01). Only two women from Dakar and two other from Kaolack were found to be HIV-1-infected. Our observations suggest a seemingly low seroprevalence of HSV-2 infection in adult women Senegal, comparable with those usually reported in Western countries. Further, epidemiological surveys are needed to confirm these results in the general population. [ABSTRACT FROM AUTHOR]

Published

2008

10. Modulation of in vitro antimalarial responses by polymorphisms in Plasmodium falciparum ABC transporters (pfmdr1 and pfmdr5).

Author

Gendrot, Mathieu, Wague Gueye, Mamadou, Tsombeng Foguim, Francis, Madamet, Marylin, Wade, Khalifa Ababacar, Bou Kounta, Mame, Fall, Mansour, Diawara, Silman, Benoit, Nicolas, Lo, Gora, Bercion, Raymond, Amalvict, Rémy, Mosnier, Joel, Fall, Bécaye, Briolant, Sébastien, Diatta, Bakary, and Pradines, Bruno

Subjects

*ATP-binding cassette transporters, *PLASMODIUM falciparum, *MULTIDRUG resistance, *HAPLOTYPES, *DRUG resistance, *AMINO acids, *ALLELES

Abstract

• Two ATP-binding cassette transporter genes (pfmdr1 and pfmdr5) sequenced in 67 P. falciparum isolates from Dakar, Senegal. • Fourteen different allelic group identified in the 67 isolates for pfmdr5. • Parasites with 8 and more than 8 repeats of DNNN motif in pfmdr5 were significantly more susceptible to piperaquine. • The wild-type allele N86 and the N86-184Y haplotype in pfmdr1 were associated with reduced susceptibility to lumefantrine. The emergence of resistance to artemisinin-based combination therapies (ACT) was described in Southeast Asia. In this context, the identification of molecular markers of ACT resistance partner drugs is urgently needed for monitoring the emergence and spread of resistance. Polymorphisms in transporter genes, especially of the ATP-binding cassette (ABC) superfamily, have been involved in anti-malarial drug resistance. In this study, the association between the mutations in the P. falciparum multidrug resistance 1 gene (pfmdr1, N86Y, Y184 F, S1034C, N1042D and D1246Y) or repetitive amino acid motifs in pfmdr5 and the ex vivo susceptibility to anti-malarial drugs was evaluated. Susceptibility to chloroquine, quinine, monodesethylamodiaquine, lumefantrine, piperaquine, pyronaridine, mefloquine and dihydroartemisinin was assessed in 67 Senegalese isolates. The shorter DNNN motif ranged from to 2 to 11 copy repeats, and the longer DHHNDHNNDNNN motif ranged from 0 to 2 in pfmdr5. The present study showed the association between repetitive amino acid motifs (DNNN-DHHNDDHNNDNNN) in pfmdr5 and in vitro susceptibility to 4-aminoquinoline-based antimalarial drugs. The parasites with 8 and more copy repeats of DNNN in pfmdr5 were significantly more susceptible to piperaquine. There was a significant association between parasites whose DHHNDHNNDNNN motif was absent and replaced by DHHNDNNN, DHHNDHNNDHNNDNNN or DHHNDHNNDHNNDHNNDNNN and increased susceptibility to chloroquine, monodesethylamodiaquine and pyronaridine. A significant association between both the wild-type allele N86 in pfmdr1 and the N86-184 F haplotype and reduced susceptibility to lumefantrine was confirmed. Further studies with a large number of samples are required to validate the association between these pfmdr5 alleles and the modulation of 4-aminoquinoline-based antimalarial drug susceptibility. [ABSTRACT FROM AUTHOR]

Published

2019

11. Absence of association between polymorphisms in the pfcoronin and pfk13 genes and the presence of Plasmodium falciparum parasites after treatment with artemisinin derivatives in Senegal.

Author

Delandre, Océane, Daffe, Sokhna M., Gendrot, Mathieu, Diallo, Maguette N., Madamet, Marylin, Kounta, Mame B., Diop, Moustapha N., Bercion, Raymond, Sow, Abdou, Ngom, Papa M., Lo, Gora, Benoit, Nicolas, Amalvict, Rémy, Fonta, Isabelle, Mosnier, Joel, Diawara, Silman, Wade, Khalifa A., Fall, Mansour, Fall, Khadidiatou B., and Fall, Bécaye

Subjects

*ARTEMISININ derivatives, *PLASMODIUM falciparum, *GENETIC mutation, *FISHER exact test, *FISH parasites

Abstract

• 348 P. falciparum samples from 327 patients collected from 2015–2019 in Hôpital Principal de Dakar, Senegal. • 16 patients (4.9%) still parasitaemic on Day 3 after t artemisinin-based combination therapy (ACT). • All sequences had wild-type pfk13 allele. • Identification of P76S mutation in pfcoronin (mean prevalence16.2%). • No significant association between in vivo reduced efficacy to ACT and P76S mutation. Due to resistance to chloroquine and sulfadoxine/pyrimethamine, treatment for uncomplicated Plasmodium falciparum malaria switched to artemisinin-based combination therapy (ACT) in 2006 in Senegal. Several mutations in the gene encoding the kelch13 helix (pfk13-propeller) have been identified as associated with in vitro and in vivo artemisinin resistance in Southeast Asia. Additionally, three mutations in the pfcoronin gene (G50E, R100K and E107V) have been identified in two culture-adapted Senegalese field isolates that became resistant in vitro to artemisinin after 4 years of intermittent selection with dihydroartemisinin. The aims of this study were to assess the prevalence of pfcoronin and pfk13 mutations in Senegalese field isolates from Dakar and to investigate their association with artemisinin derivative clinical failures. A total of 348 samples of P. falciparum from 327 patients, collected from 2015–2019 in Dakar, were successfully analysed. All sequences had wild-type pfk13 allele. The three mutations (G50E, R100K and E107V), previously identified in parasites with reduced susceptibility to artemisinin, were not found in this study, but a new mutation (P76S) was detected (mean prevalence 16.2%). The P76S mutation was identified in 5 (31.3%) of 16 isolates collected from patients still parasitaemic on Day 3 after ACT treatment and in 31 samples (15.3%) among 203 patients considered successfully cured. There was no significant association between in vivo reduced efficacy to artemisinin derivatives and the P76S mutation (P = 0.151, Fisher's exact test). These data suggest that polymorphisms in pfk13 and pfcoronin are not the best predictive markers for artemisinin resistance in Senegal. [ABSTRACT FROM AUTHOR]

Published

2020