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   Short-term forecasting of the prevalence of clinical trachoma: Utility of including delayed recovery and tests for infection  
   
نویسنده liu f. ,porco t.c. ,amza a. ,kadri b. ,nassirou b. ,west s.k. ,bailey r.l. ,keenan j.d. ,lietman t.m.
منبع parasites and vectors - 2015 - دوره : 8 - شماره : 1
چکیده    Background: the world health organization aims to control blinding trachoma by 2020. decisions on whether to start and stop mass treatments and when to declare that control has been achieved are currently based on clinical examination data generated in population-based surveys. thresholds are based on the district-level prevalence of trachomatous inflammation-follicular (tf) in children aged 1-9 years. forecasts of which districts may and may not meet tf control goals by the 2020 target date could affect resource allocation in the next few years. methods: we constructed a hidden markov model fit to the prevalence of two clinical signs of trachoma and pcr data in 24 communities from the recent pret-niger trial. the prevalence of tf in children in each community at 36 months was forecast given data from earlier time points. forecasts were scored by the likelihood of the observed results. we assessed whether use of tf with additional ti and pcr data rather than just the use of tf alone improves forecasts,and separately whether incorporating a delay in tf recovery is beneficial. results: including ti and pcr data did not significantly improve forecasts of tf. forecasts of tf prevalence at 36 months by the model with the delay in tf recovery were significantly better than forecasts by the model without the delay in tf recovery (p∈=∈0.003). a zero-inflated truncated normal observation model was better than a truncated normal observation model,and better than a sensitivity-specificity observation model. conclusion: the results in this study suggest that future studies could consider using just tf data for forecasting,and should include a delay in tf recovery. trial registration: clinicaltrials.gov nct00792922 © 2015 liu et al.
کلیدواژه Forecast; Mass drug administration; Model; Prediction; Trachoma
آدرس f.i. proctor foundation,university of california san francisco,medical sciences 309a,513 parnassus,san francisco,ca 94143-0944, United States, f.i. proctor foundation,university of california san francisco,medical sciences 309a,513 parnassus,san francisco,ca 94143-0944,united states,department of ophthalmology,university of california san francisco,san francisco,ca,united states,department of epidemiology and biostatistics,university of california san francisco,san francisco,ca, United States, programme fss/université abdou moumouni de niamey,programme national de santé oculaire,niamey, Niger, programme fss/université abdou moumouni de niamey,programme national de santé oculaire,niamey, Niger, programme fss/université abdou moumouni de niamey,programme national de santé oculaire,niamey, Niger, dana center for preventive ophthalmology,wilmer eye institute,johns hopkins university,baltimore,md, United States, clinical research unit,department of infectious and tropical diseases,london school of hygiene and tropical medicine,london, United Kingdom, f.i. proctor foundation,university of california san francisco,medical sciences 309a,513 parnassus,san francisco,ca 94143-0944,united states,department of ophthalmology,university of california san francisco,san francisco,ca, United States, f.i. proctor foundation,university of california san francisco,medical sciences 309a,513 parnassus,san francisco,ca 94143-0944,united states,department of ophthalmology,university of california san francisco,san francisco,ca,united states,department of epidemiology and biostatistics,university of california san francisco,san francisco,ca, United States
 
     
   
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