Your search keyword '"Nassirou, Beido"' showing total 4 results

1. Monitoring transmission intensity of trachoma with serology: a multi-country study

Author

Tedijanto, Christine, Solomon, Anthony W., Martin, Diana L., Nash, Scott D., Keenan, Jeremy D., Lietman, Thomas M., Lammie, Patrick J., Aiemjoy, Kristen, Amza, Abdou, Aragie, Solomon, Arzika, Ahmed M., Callahan, E. Kelly, Carolan, Sydney, Dawed, Adisu Abebe, Goodhew, E. Brook, Gwyn, Sarah, Hammou, Jaouad, Kadri, Boubacar, Kalua, Khumbo, Maliki, Ramatou, Nassirou, Beido, Seife, Fikre, Tadesse, Zerihun, West, Sheila K., Wittberg, Dionna M., Zeru, Taye, and Arnold, Benjamin F.

Subjects

Article

Abstract

Trachoma, caused by ocular Chlamydia trachomatis infection, is targeted for global elimination as a public health problem by 2030. To provide evidence for use of antibodies to monitor C. trachomatis transmission, we collated IgG responses to Pgp3 antigen, PCR positivity, and clinical observations from 19,811 children aged 1–9 years in 14 populations. We demonstrate that age-seroprevalence curves consistently shift along a gradient of transmission intensity: rising steeply in populations with high levels of infection and active trachoma and becoming flat in populations near elimination. Seroprevalence (range: 0–54%) and seroconversion rates (range: 0–15 per 100 person-years) correlate with PCR prevalence (r: 0.88, 95% CI: 0.77, 0.93). A seroprevalence threshold of 13.5% (seroconversion rate 2.75 per 100 person-years) identifies clusters with any infection at high sensitivity (>90%) and moderate specificity (69-75%). Antibody responses in young children provide a robust, generalizable approach to monitor population progress toward and beyond trachoma elimination.

Published

2023

2. Cause-specific mortality of children younger than 5 years in communities receiving biannual mass azithromycin treatment in Niger: verbal autopsy results from a cluster-randomised controlled trial

Author

Jeremy D Keenan, Ahmed M Arzika, Ramatou Maliki, Sanoussi Elh Adamou, Fatima Ibrahim, Mariama Kiemago, Nana Fatima Galo, Elodie Lebas, Catherine Cook, Benjamin Vanderschelden, Robin L Bailey, Sheila K West, Travis C Porco, Thomas M Lietman, Paul M Emerson, Jerusha Weaver, John Hart, Amza Abdou, Boubacar Kadri, Nassirou Beido, E Kelly Callahan, Aisha E Stewart, Salissou Kane, Sun Y Cotter, Thuy Doan, Dionna M Fry, Ying Lin, Kieran S O'Brien, Catherine E Oldenburg, Kathryn J Ray, Philip J Rosenthal, George W Rutherford, Nicole E Varnado, Lina Zhong, and Zhaoxia Zhou

Subjects

Male, Pediatrics, medicine.medical_specialty, 030231 tropical medicine, Population, Azithromycin, Placebo, Rate ratio, Antimalarials, 03 medical and health sciences, 0302 clinical medicine, Cause of Death, Infant Mortality, medicine, Cluster Analysis, Humans, Niger, 030212 general & internal medicine, education, Cause of death, education.field_of_study, business.industry, lcsh:Public aspects of medicine, Infant, Newborn, Infant, lcsh:RA1-1270, General Medicine, Verbal autopsy, Infant mortality, Anti-Bacterial Agents, Malaria, Child mortality, Child, Preschool, Child Mortality, Mass Drug Administration, Female, business, medicine.drug

Abstract

Summary Background The Macrolides Oraux pour Reduire les Deces avec un Oeil sur la Resistance (MORDOR) trial found that biannual mass distribution of azithromycin to children younger than 5 years in Niger reduced the primary outcome of all-cause mortality by 18%. We aimed to determine the causes of mortality among deceased children using verbal autopsy. Methods In this 2-year cluster-randomised controlled trial, 594 community clusters in Niger were randomly allocated (1:1 ratio) to receive biannual mass distributions of either oral azithromycin (approximately 20 mg per kg of bodyweight) or placebo targeted to children aged 1–59 months. Participants, study investigators, and field workers were masked to treatment allocation. Between Nov 23, 2014, and July 31, 2017, 3615 child deaths were recorded by use of biannual house-to-house censuses, and verbal autopsies were done between May 26, 2015, and May 17, 2018, to identify cause of death. Cause-specific mortality, as assessed by verbal autopsy, was a prespecified secondary outcome. This trial is completed and is registered with ClinicalTrials.gov , NCT02047981 . Findings Between Nov 23, 2014, and July 31, 2017, 303 communities (n=40 375 children at baseline) in Niger received mass azithromycin and 291 communities (n=35 747 children at baseline) received placebo. Treatment coverage was 90·3% (SD 10·6) in the azithromycin group and 90·4% (10·1) in the placebo group. No communities were lost to follow-up. In total, 1727 child deaths in the azithromycin group and 1888 child deaths in the placebo group were reported from the population censuses. Of these, the cause of death for 1566 (90·7%) children in the azithromycin group and 1735 (91·9%) children in the placebo group were ascertained by verbal autopsy interviews. In the azithromycin group, 437 (27·9%) deaths were due to malaria, 252 (16·1%) deaths were due to pneumonia, and 234 (14·9%) deaths were due to diarrhoea. In the placebo group, 493 (28·4%) deaths were due to malaria, 275 (15·9%) deaths were due to pneumonia, and 251 (14·5%) deaths were due to diarrhoea. Relative to communities that received placebo, child mortality in communities that received azithromycin was lower for malaria (incidence rate ratio 0·78, 95% CI 0·66–0·92; p=0·0029), dysentery (0·65, 0·44–0·94; p=0·025), meningitis (0·67, 0·46–0·97; p=0·036), and pneumonia (0·83, 0·68–1·00; p=0·051). The distribution of causes of death did not differ significantly between the two study groups (p=0·98). Interpretation Mass azithromycin distribution resulted in approximately a third fewer deaths in children aged 1–59 months due to meningitis and dysentery, and a fifth fewer deaths due to malaria and pneumonia. The lack of difference in the distribution of causes of death between the azithromycin and placebo groups could be attributable to the broad spectrum of azithromycin activity and the study setting, in which most childhood deaths were due to infections. Funding Bill & Melinda Gates Foundation.

Published

2020

3. Effectiveness of expanding annual mass azithromycin distribution treatment coverage for trachoma in Niger: a cluster randomised trial

Author

Amza, Abdou, Kadri, Boubacar, Nassirou, Beido, Cotter, Sun Y, Stoller, Nicole E, West, Sheila K, Bailey, Robin L, Porco, Travis C, Gaynor, Bruce D, Keenan, Jeremy D, Lietman, Thomas M, and Oldenburg, Catherine E

Subjects

Male, Clinical Trials and Supportive Activities, Clinical Sciences, Azithromycin, Ophthalmology & Optometry, Clinical Research, Opthalmology and Optometry, Prevalence, Humans, Niger, Child, Preschool, Eye Disease and Disorders of Vision, Trachoma, Child Health, Infant, Antibiotic Prophylaxis, Clinical Trial, Anti-Bacterial Agents, Infectious Diseases, Good Health and Well Being, Cost Effectiveness Research, Public Health and Health Services, Female, Public Health, Infection, Delivery of Health Care, Conjunctiva

Abstract

Background/aimsThe WHO recommends 3-5 years of annual mass azithromycin distribution with at least 80% treatment coverage to districts with active trachoma prevalence over 10% among children. Here, we assess the efficacy of expanding the coverage target to at least 90% for trachoma control in a mesoendemic region of Niger.MethodsTwenty-four communities were randomised to a single day of azithromycin distribution with a coverage target of 80% of the community or up to 4 days of treatment, aiming for greater than 90% coverage. Distributions were annual and individuals above 6 months of age were treated. Children under 5 years of age were monitored for ocular chlamydia infection and active trachoma.ResultsAt baseline, ocular chlamydia prevalence was 20.5% (95% CI 9.8% to 31.2%) in the standard coverage arm and 21.9% (95% CI 11.3% to 32.5%) in the enhanced coverage arm, which reduced to 4.6% (95% CI 0% to 9.5%, p=0.008) and 7.1% (95% CI 2.7% to 11.4%, p

Published

2018

4. Application of smartphone cameras for detecting clinically active trachoma: Table 1

Author

Thomas M. Lietman, Satasuk Joy Bhosai, Jeremy D. Keenan, Bruce D. Gaynor, Robin L. Bailey, Abdou Amza, and Nassirou Beido

Subjects

business.industry, medicine.disease, Field training, Sensory Systems, Cellular and Molecular Neuroscience, Ophthalmology, Trachoma, Research studies, Medicine, Mass treatment, Optometry, Continuity of care, Mobile technology, business

Abstract

The WHO is committed to eliminating trachoma as a public health concern by 2020.1 Since decisions for mass treatment are determined by the prevalence of clinical trachoma in a community, efficient and accurate methods for monitoring clinical activity remain a priority.2 However, reliability of clinical examination is poor and disagreement between graders is common.3 Photography of the conjunctiva could reduce variability and improve accuracy of trachoma surveillance. Currently, research studies use single-lens reflex (SLR) cameras to validate field grading.4 Yet, SLR cameras are expensive and require substantial field training to operate, and thus few trachoma programmes have adopted this technology. A simpler, more affordable camera may increase uptake of this diagnostic technique. In view of growing applications of mobile technology,5 we examined the use of smartphone imaging in trachoma. During a recent programme, Partnership for the Rapid Elimination of Trachoma (PRET study) visit in Niger, we performed …

Published

2012