5 results on '"Kamal Said Abdallah"'
Search Results
2. Artemisinin-piperaquine versus artemether-lumefantrine for treatment of uncomplicated Plasmodium falciparum malaria in Grande Comore island: an open-label, non-randomised controlled trial
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Guoming Li, Yueming Yuan, Shaoqin Zheng, Chenguang Lu, Mingqiang Li, Ruixiang Tan, Hongying Zhang, Rahamatou Silai, Ruimei Liu, Kamal Said Abdallah, Affane Bacar, Qin Xu, Jianping Song, Wanting Wu, and Changsheng Deng
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Microbiology (medical) ,Fluorenes ,Artemether, Lumefantrine Drug Combination ,Plasmodium falciparum ,General Medicine ,Artemisinins ,Piperazines ,Malaria ,Antimalarials ,Drug Combinations ,Infectious Diseases ,Ethanolamines ,Quinolines ,Humans ,Pharmacology (medical) ,Artemether ,Malaria, Falciparum - Abstract
Malaria significantly rebounded in 2018 in the Comoros; this created an urgent need to conduct clinical trials to investigate the effectiveness of artemisinin and its derivatives.An open-label, non-randomised controlled trial of artemisinin-piperaquine (AP) and artemether-lumefantrine (AL) was conducted in Grande Comore island from June 2019 to January 2020. A total of 238 uncomplicated falciparum malaria cases were enrolled and divided 1:1 into two treatments. The primary endpoint was the 42-day adequate clinical and parasitological responses (ACPR). Secondary endpoints were parasitaemia and fever clearance at day 3, gametocytes and tolerability.The 42-day ACPR before and after PCR correction were 91.43% (95% CI 83.93-95.76%) and 98.06% (95% CI 92.48-99.66%) for AP treatment, respectively, and 96.00% (95% CI 88.17-98.14%) and 98.97% (95% CI 93.58-99.95%) for AL treatment, respectively. Complete clearance of the parasitaemia and fever for both groups was detected on day 3. Gametocytes disappeared on day 21 in the AP group and on day 2 in AL group. Specifically, the adverse reactions were mild in both groups.It was found that AP and AL maintained their high efficacy and tolerance in the Comoros. Nonetheless, asymptomatic malaria infections bring new challenges to malaria control.
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- 2022
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3. Detection of SARS-CoV-2 variant 501Y.V2 in Comoros Islands in January 2021
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George Githinji, Ali Ahmed Yahaya, Edward Otieno, Peter Borus, Charles N. Agoti, James D. Nokes, Benjamin Tsofa, Dratibi Fred Athanasius, Nicksy Gumede-Moeletsi, Kamal Said Abdallah, Arnold W. Lambisia, Edidah M. Ong'era, Abdoulaye Diarra, Khadija Said Mohammed, Zaydah R. de Laurent, John M. Morobe, Hamza Abdou Yahaya, Philip Bejon, Isabella Lynette Ocholla, and Maureen W. Mburu
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0301 basic medicine ,Most recent common ancestor ,2019-20 coronavirus outbreak ,Overseas department ,Lineage (genetic) ,Coronavirus disease 2019 (COVID-19) ,Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) ,030106 microbiology ,Medicine (miscellaneous) ,Biology ,Genome ,General Biochemistry, Genetics and Molecular Biology ,Comoros ,03 medical and health sciences ,Pandemic ,501Y.V2 ,geography ,geography.geographical_feature_category ,Phylogenetic tree ,SARS-CoV-2 ,Articles ,Virology ,Research Note ,030104 developmental biology ,Evolutionary biology ,Archipelago - Abstract
Background. Genomic data is key in understanding the spread and evolution of SARS-CoV-2 pandemic and informing the design and evaluation of interventions. However, SARS-CoV-2 genomic data remains scarce across Africa, with no reports yet from the Indian Ocean islands. Methods. We genome sequenced six SARS-CoV-2 positive samples from the first major infection wave in the Union of Comoros in January 2021 and undertook detailed phylogenetic analysis. Results. All the recovered six genomes classified within the 501Y.V2 variant of concern (also known as lineage B.1.351) and appeared to be from 2 sub-clusters with the most recent common ancestor dated 30th Oct-2020 (95% Credibility Interval: 06th Sep-2020 to 10th Dec-2020). Comparison of the Comoros genomes with those of 501Y.V2 variant of concern from other countries deposited into the GISAID database revealed their close association with viruses identified in France and Mayotte (part of the Comoros archipelago and a France, Overseas Department). Conclusions. The recovered genomes, albeit few, confirmed local transmission following probably multiple introductions of the SARS-CoV-2 501Y.V2 variant of concern during the Comoros’s first major COVID-19 wave. These findings demonstrate the importance of genomic surveillance and have implications for ongoing control strategies on the islands.
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- 2021
4. Large-scale Artemisinin–Piperaquine Mass Drug Administration With or Without Primaquine Dramatically Reduces Malaria in a Highly Endemic Region of Africa
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Xiaobo Li, Fouad Mohadji, Hong Yan, Xiao-Hong Liu, Di Li, Danghong Feng, Kamal Said Abdallah, Guoming Li, Fei Tuo, Shaoqin Zheng, Ahamada M. S. A. Mliva, Changsheng Deng, Xinhua Wang, Xin-zhuan Su, Linlu Xue, Qi Wang, Michael P. Fay, Hongying Zhang, Bo Huang, Li Lin, Thomas E. Wellems, Zhibing Wu, Moussa Mohamed, Rachadi A Kéké, Wanting Wu, Jianping Song, Shiguang Huang, Fangli Lu, Qin Xu, Fatihou Oithik, Jiuyao Zhou, Affane Bacar, and Tao Yang
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Male ,Primaquine ,Endemic Diseases ,Parasitemia ,Comoros ,0302 clinical medicine ,030212 general & internal medicine ,Malaria, Falciparum ,Artemisinin ,Child ,Articles and Commentaries ,education.field_of_study ,biology ,Artemisinins ,Treatment Outcome ,Infectious Diseases ,Child, Preschool ,Quinolines ,Mass Drug Administration ,Drug Therapy, Combination ,Female ,medicine.drug ,Adult ,Microbiology (medical) ,medicine.medical_specialty ,Adolescent ,Plasmodium falciparum ,030231 tropical medicine ,Population ,Antimalarials ,Young Adult ,03 medical and health sciences ,Internal medicine ,Piperaquine ,parasitic diseases ,medicine ,Humans ,Mass drug administration ,education ,Polymorphism, Genetic ,business.industry ,Infant ,DNA, Protozoan ,medicine.disease ,biology.organism_classification ,business ,Malaria - Abstract
BACKGROUND: Mass drug administration (MDA), with or without low-dose primaquine (PMQ(LD)), is being considered for malaria elimination programs. The potential of PMQ(LD) to block malaria transmission by mosquitoes must be balanced against liabilities of its use. METHODS: Artemisinin–piperaquine (AP), with or without PMQ(LD), was administered in 3 monthly rounds across Anjouan Island, Union of Comoros. Plasmodium falciparum malaria rates, mortality, parasitemias, adverse events, and PfK13 Kelch-propeller gene polymorphisms were evaluated. RESULTS: Coverage of 85 to 93% of the Anjouan population was achieved with AP plus PMQ(LD) (AP+PMQ(LD)) in 2 districts (population 97164) and with AP alone in 5 districts (224471). Between the months of April–September in both 2012 and 2013, average monthly malaria hospital rates per 100000 people fell from 310.8 to 2.06 in the AP+PMQ(LD) population (ratio 2.06/310.8 = 0.66%; 95% CI: 0.02%, 3.62%; P = .00007) and from 412.1 to 2.60 in the AP population (ratio 0.63%; 95% CI: 0.11%, 1.93%; P < .00001). Effectiveness of AP+PMQ(LD) was 0.9908 (95% CI: 0.9053, 0.9991), while effectiveness of AP alone was 0.9913 (95% CI: 0.9657, 0.9978). Both regimens were well tolerated, without severe adverse events. Analysis of 52 malaria samples after MDA showed no evidence for selection of PfK13 Kelch-propeller mutations. CONCLUSIONS: Steep reductions of malaria cases were achieved by 3 monthly rounds of either AP+PMQ(LD) or AP alone, suggesting potential for highly successful MDA without PMQ(LD) in epidemiological settings such as those on Anjouan. A major challenge is to sustain and expand the public health benefits of malaria reductions by MDA.
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- 2018
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5. Temporal changes in genetic diversity of msp-1, msp-2, and msp-3 in Plasmodium falciparum isolates from Grande Comore Island after introduction of ACT
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Qin Xu, Shaoqin Zheng, Zhaoli Yang, Wang Qi, Fei Tuo, Affane Bacar, Shiguang Huang, Kamal Said Abdallah, Changsheng Deng, Qirun Zhong, Guangchao Wu, Bo Huang, Wanting Wu, Jianping Song, Ahamada M. S. A. Mliva, Hongying Zhang, Xin-zhuan Su, Yuan Liang, and Mingqiang Li
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0301 basic medicine ,lcsh:Arctic medicine. Tropical medicine ,lcsh:RC955-962 ,030231 tropical medicine ,Plasmodium falciparum ,Protozoan Proteins ,Antigens, Protozoan ,Biology ,Comoros ,Genetic diversity ,lcsh:Infectious and parasitic diseases ,03 medical and health sciences ,Antimalarials ,0302 clinical medicine ,Multiplicity of infection ,parasitic diseases ,medicine ,Humans ,lcsh:RC109-216 ,DNA sequencing ,Allele ,Merozoite surface protein ,Grande Comore ,Genotyping ,Merozoite Surface Protein 1 ,Genetics ,Research ,Malaria population ,Genetic Variation ,medicine.disease ,biology.organism_classification ,Artemisinins ,030104 developmental biology ,Infectious Diseases ,PCR ,Parasitology ,Drug Therapy, Combination ,Nested polymerase chain reaction ,Malaria - Abstract
Background Malaria is still one of the serious public health problems in Grande Comore Island, although the number of annual cases has been greatly reduced in recent years. A better understanding of malaria parasite population diversity and transmission dynamics is critical for assessing the effectiveness of malaria control measures. The objective of this study is to investigate temporal changes in genetic diversity of Plasmodium falciparum populations and multiplicity of infection (MOI) in Grande Comore 10 years after introduction of ACT. Methods A total of 232 P. falciparum clinical isolates were collected from the Grande Comore Island during two sampling periods (118 for 2006‒2007 group, and 114 for 2013‒2016 group). Parasite isolates were characterized for genetic diversity and complexity of infection by genotyping polymorphic regions in merozoite surface protein gene 1 (msp-1), msp-2, and msp-3 using nested PCR and DNA sequencing. Results Three msp-1 alleles (K1, MAD20, and RO33), two msp-2 alleles (FC27 and 3D7), and two msp-3 alleles (K1 and 3D7) were detected in parasites of both sampling periods. The RO33 allele of msp-1 (84.8%), 3D7 allele of msp-2 (90.8%), and K1 allele of msp-3 (66.7%) were the predominant allelic types in isolates from 2006–2007 group. In contrast, the RO33 allele of msp-1 (63.4%), FC27 allele of msp-2 (91.1%), and 3D7 allele of msp-3 (53.5%) were the most prevalent among isolates from the 2013–2016 group. Compared with the 2006‒2007 group, polyclonal infection rates of msp-1 (from 76.7 to 29.1%, P
- Published
- 2017
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