Your search keyword '"H. Osvaldo Aurelio"' showing total 3 results

1. Protocol and baseline data for a multi-year cohort study of the effects of different mass drug treatment approaches on functional morbidities from schistosomiasis in four African countries

Author

Ye Shen, Charles H. King, Sue Binder, Feng Zhang, Christopher C. Whalen, W. Evan Secor, Susan P. Montgomery, Pauline N. M. Mwinzi, Annette Olsen, Pascal Magnussen, Safari Kinung’hi, Anna E. Phillips, Rassul Nalá, Josefo Ferro, H. Osvaldo Aurelio, Fiona Fleming, Amadou Garba, Amina Hamidou, Alan Fenwick, Carl H. Campbell, and Daniel G. Colley

Subjects

Schistosomiasis, Schistosoma haematobium, Schistosoma mansoni, Morbidity, Drug therapy, Praziquantel, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background The Schistosomiasis Consortium for Operational Research and Evaluation (SCORE) focus is on randomized trials of different approaches to mass drug administration (MDA) in endemic countries in Africa. Because their studies provided an opportunity to evaluate the effects of mass treatment on Schistosoma-associated morbidity, nested cohort studies were developed within SCORE’s intervention trials to monitor changes in a suite of schistosomiasis disease outcomes. This paper describes the process SCORE used to select markers for prospective monitoring and the baseline prevalence of these morbidities in four parallel cohort studies. Methods In July 2009, SCORE hosted a discussion of the potential impact of MDA on morbidities due to Schistosoma infection that might be measured in the context of multi-year control. Candidate markers were reviewed and selected for study implementation. Baseline data were then collected from cohorts of children in four country studies: two in high endemic S. mansoni sites (Kenya and Tanzania), and two in high endemic S. haematobium sites (Niger and Mozambique), these cohorts to be followed prospectively over 5 years. Results At baseline, 62% of children in the S. mansoni sites had detectable eggs in their stool, and 10% had heavy infections (≥ 400 eggs/g feces). Heavy S. mansoni infections were found to be associated with increased baseline risk of anemia, although children with moderate or heavy intensity infections had lower risk of physical wasting. Prevalence of egg-positive infection in the combined S. haematobium cohorts was 27%, with 5% of individuals having heavy infection (≥50 eggs/10 mL urine). At baseline, light intensity S. haematobium infection was associated with anemia and with lower scores in the social domain of health-related quality-of-life (HRQoL) assessed by Pediatric Quality of Life Inventory. Conclusions Our consensus on practical markers of Schistosoma-associated morbidity indicated that height, weight, hemoglobin, exercise tolerance, HRQoL, and ultrasound abnormalities could be used as reference points for gauging treatment impact. Data collected over five years of program implementation will provide guidance for future evaluation of morbidity control in areas endemic for schistosomiasis. Trial registration These cohort studies are registered and performed in conjunction with the International Standard Randomised Controlled Trial Registry trials ISRCTN16755535 , ISRCTN14117624 , ISRCTN95819193 , and ISRCTN32045736 .

Published

2017

2. Modelling control of Schistosoma haematobium infection: predictions of the long-term impact of mass drug administration in Africa

Author

David Gurarie, Nara Yoon, Emily Li, Martial Ndeffo-Mbah, David Durham, Anna E. Phillips, H. Osvaldo Aurelio, Josefo Ferro, Alison P. Galvani, and Charles H. King

Subjects

Mathematical models, Theoretical/parasitology, Schistosomiasis/prevention and control, Drug therapy/organization and administration, Disease transmission, Infectious disease, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background Effective control of schistosomiasis remains a challenging problem for endemic areas of the world. Given knowledge of the biology of transmission and past experience with mass drug administration (MDA) programs, it is important to critically evaluate the likelihood that MDA programs will achieve substantial reductions in Schistosoma prevalence. In implementing the World Health Organization Roadmap for Neglected Tropical Diseases it would useful for policymaking to model projections of the status of Schistosoma control in MDA-treated areas in the next 5–10 years. Methods Calibrated mathematical models were used to project the effects of different frequency and coverage of MDA for schistosomiasis haematobia control in present-day endemic communities, taking into account uncertainties of parasite biology and input data. The modeling approach in this analysis was the Stratified Worm Burden model developed in our earlier works, calibrated using data from longitudinal S. haematobium control trials in Kenya. Results Model-based simulations of MDA control in typical low-risk and higher-risk communities indicated that infection prevalence can be substantially reduced within 10 years only when there is a high degree of community participation (>70 %) with at least annual MDA. Significant risk for re-emergence of infection remains if MDA is suspended. Conclusions In a stable (stationary) ecosystem, Schistosoma reproduction and transmission are sufficiently robust that the process of human infection continues, even under pressure from aggressive MDA. MDA alone is unlikely to interrupt transmission, and once mass treatment is suspended, the prevalence of human infection is likely to rebound to pre-control levels over a period of 25–30 years. MDA success in achieving very low levels of infection prevalence is highly dependent on treatment coverage and frequency within the local human population, and requires that both adults and children be included in drug delivery coverage. Ultimately, supplemental snail control and significant improvements in sanitation will be required to achieve full control of schistosomiasis by elimination of ongoing Schistosoma transmission.

Published

2015

3. Modelling control of Schistosoma haematobium infection: predictions of the long-term impact of mass drug administration in Africa

Author

Charles H. King, Emily Li, David Gurarie, Nara Yoon, Alison P. Galvani, Josefo Ferro, Martial L. Ndeffo-Mbah, H. Osvaldo Aurelio, David P. Durham, and Anna E. Phillips

Subjects

Adult, Male, Veterinary medicine, Time Factors, Sanitation, Disease transmission, Population, Mycology & Parasitology, Schistosomiasis, Praziquantel, Drug therapy/organization and administration, Schistosomiasis haematobia, 1108 Medical Microbiology, Environmental health, medicine, Animals, Humans, Mass drug administration, education, Schistosoma, Anthelmintics, Schistosoma haematobium, Mathematical models, Theoretical/parasitology, Infectious disease, education.field_of_study, biology, Research, Models, Theoretical, medicine.disease, biology.organism_classification, Infectious Diseases, 1117 Public Health And Health Services, Africa, Neglected tropical diseases, Female, Parasitology, Schistosomiasis/prevention and control, medicine.drug

Abstract

Background Effective control of schistosomiasis remains a challenging problem for endemic areas of the world. Given knowledge of the biology of transmission and past experience with mass drug administration (MDA) programs, it is important to critically evaluate the likelihood that MDA programs will achieve substantial reductions in Schistosoma prevalence. In implementing the World Health Organization Roadmap for Neglected Tropical Diseases it would useful for policymaking to model projections of the status of Schistosoma control in MDA-treated areas in the next 5–10 years. Methods Calibrated mathematical models were used to project the effects of different frequency and coverage of MDA for schistosomiasis haematobia control in present-day endemic communities, taking into account uncertainties of parasite biology and input data. The modeling approach in this analysis was the Stratified Worm Burden model developed in our earlier works, calibrated using data from longitudinal S. haematobium control trials in Kenya. Results Model-based simulations of MDA control in typical low-risk and higher-risk communities indicated that infection prevalence can be substantially reduced within 10 years only when there is a high degree of community participation (>70 %) with at least annual MDA. Significant risk for re-emergence of infection remains if MDA is suspended. Conclusions In a stable (stationary) ecosystem, Schistosoma reproduction and transmission are sufficiently robust that the process of human infection continues, even under pressure from aggressive MDA. MDA alone is unlikely to interrupt transmission, and once mass treatment is suspended, the prevalence of human infection is likely to rebound to pre-control levels over a period of 25–30 years. MDA success in achieving very low levels of infection prevalence is highly dependent on treatment coverage and frequency within the local human population, and requires that both adults and children be included in drug delivery coverage. Ultimately, supplemental snail control and significant improvements in sanitation will be required to achieve full control of schistosomiasis by elimination of ongoing Schistosoma transmission. Electronic supplementary material The online version of this article (doi:10.1186/s13071-015-1144-3) contains supplementary material, which is available to authorized users.