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Impact of Introducing Hepatitis B Birth Dose Vaccines into the Infant Immunization Program in Burkina Faso: Study Protocol for a Stepped Wedge Cluster Randomized Trial (NéoVac Study)

To achieve global hepatitis elimination by 2030, it is critical to prevent the mother-to-child transmission (MTCT) of hepatitis B virus (HBV). Since 2009, the WHO has recommended administering hepatitis B vaccine to all neonates within 24 h of birth to prevent MTCT. However, many countries in sub-Sa...

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Autores principales: Tall, Haoua, Adam, Pierrick, Tiendrebeogo, Abdoul Salam Eric, Vincent, Jeanne Perpétue, Schaeffer, Laura, von Platen, Cassandre, Fernandes-Pellerin, Sandrine, Sawadogo, François, Bokoum, Alkadri, Bouda, Ghislain, Ouattara, Seydou, Ouédraogo, Issa, Herrant, Magali, Boucheron, Pauline, Sawadogo, Appolinaire, Betsem, Edouard, Essoh, Alima, Kabore, Lassané, Ouattara, Amariane, Méda, Nicolas, Hien, Hervé, Gosset, Andréa, Giles-Vernick, Tamara, Boyer, Sylvie, Kania, Dramane, Vray, Muriel, Shimakawa, Yusuke
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8227098/
https://www.ncbi.nlm.nih.gov/pubmed/34206058
http://dx.doi.org/10.3390/vaccines9060583
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author Tall, Haoua
Adam, Pierrick
Tiendrebeogo, Abdoul Salam Eric
Vincent, Jeanne Perpétue
Schaeffer, Laura
von Platen, Cassandre
Fernandes-Pellerin, Sandrine
Sawadogo, François
Bokoum, Alkadri
Bouda, Ghislain
Ouattara, Seydou
Ouédraogo, Issa
Herrant, Magali
Boucheron, Pauline
Sawadogo, Appolinaire
Betsem, Edouard
Essoh, Alima
Kabore, Lassané
Ouattara, Amariane
Méda, Nicolas
Hien, Hervé
Gosset, Andréa
Giles-Vernick, Tamara
Boyer, Sylvie
Kania, Dramane
Vray, Muriel
Shimakawa, Yusuke
author_facet Tall, Haoua
Adam, Pierrick
Tiendrebeogo, Abdoul Salam Eric
Vincent, Jeanne Perpétue
Schaeffer, Laura
von Platen, Cassandre
Fernandes-Pellerin, Sandrine
Sawadogo, François
Bokoum, Alkadri
Bouda, Ghislain
Ouattara, Seydou
Ouédraogo, Issa
Herrant, Magali
Boucheron, Pauline
Sawadogo, Appolinaire
Betsem, Edouard
Essoh, Alima
Kabore, Lassané
Ouattara, Amariane
Méda, Nicolas
Hien, Hervé
Gosset, Andréa
Giles-Vernick, Tamara
Boyer, Sylvie
Kania, Dramane
Vray, Muriel
Shimakawa, Yusuke
author_sort Tall, Haoua
collection PubMed
description To achieve global hepatitis elimination by 2030, it is critical to prevent the mother-to-child transmission (MTCT) of hepatitis B virus (HBV). Since 2009, the WHO has recommended administering hepatitis B vaccine to all neonates within 24 h of birth to prevent MTCT. However, many countries in sub-Saharan Africa only provide hepatitis B immunization at the age of 6, 10, and 14 weeks or 8, 12, and 16 weeks using a combined vaccine. To accelerate the introduction of the hepatitis B birth dose vaccine (HepB-BD) into sub-Saharan Africa, it is critical to establish to what extent the addition of HepB-BD can further reduce HBV transmission in areas where three-dose infant vaccination has been implemented. We therefore designed a study to evaluate the impact, acceptability, and cost-effectiveness of incorporating the HepB-BD into the routine immunization program in a real-life field condition in Burkina Faso, where the hepatitis B vaccination is currently scheduled at 8-12-16 weeks. Through a multidisciplinary approach combining epidemiology, anthropology, and health economics, the Neonatal Vaccination against Hepatitis B in Africa (NéoVac) study conducts a pragmatic stepped wedge cluster randomized controlled trial in rural areas of the Hauts-Bassins Region. The study was registered in ClinicalTrials.gov (identifier: NCT04029454). A health center is designated as a cluster, and the introduction of HepB-BD will be rolled out sequentially in 24 centers. Following an initial period in which no health center administers HepB-BD, one center will be randomly allocated to incorporate HepB-BD. Then, at a regular interval, another center will be randomized to cross from the control to the intervention period, until all 24 centers integrate HepB-BD. Pregnant women attending antenatal care will be systematically invited to participate. Infants born during the control period will follow the conventional immunization schedule (8-12-16 weeks), while those born in the interventional period will receive HepB-BD in addition to the routine vaccines (0-8-12-16 weeks). The primary outcome, the proportion of hepatitis B surface antigen (HBsAg) positivity in infants aged at 9 months, will be compared between children born before and after HepB-BD introduction. The study will generate data that may assist governments and stakeholders in sub-Saharan Africa to make evidence-based decisions about whether to add HepB-BD into the national immunization programs.
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spelling pubmed-82270982021-06-26 Impact of Introducing Hepatitis B Birth Dose Vaccines into the Infant Immunization Program in Burkina Faso: Study Protocol for a Stepped Wedge Cluster Randomized Trial (NéoVac Study) Tall, Haoua Adam, Pierrick Tiendrebeogo, Abdoul Salam Eric Vincent, Jeanne Perpétue Schaeffer, Laura von Platen, Cassandre Fernandes-Pellerin, Sandrine Sawadogo, François Bokoum, Alkadri Bouda, Ghislain Ouattara, Seydou Ouédraogo, Issa Herrant, Magali Boucheron, Pauline Sawadogo, Appolinaire Betsem, Edouard Essoh, Alima Kabore, Lassané Ouattara, Amariane Méda, Nicolas Hien, Hervé Gosset, Andréa Giles-Vernick, Tamara Boyer, Sylvie Kania, Dramane Vray, Muriel Shimakawa, Yusuke Vaccines (Basel) Article To achieve global hepatitis elimination by 2030, it is critical to prevent the mother-to-child transmission (MTCT) of hepatitis B virus (HBV). Since 2009, the WHO has recommended administering hepatitis B vaccine to all neonates within 24 h of birth to prevent MTCT. However, many countries in sub-Saharan Africa only provide hepatitis B immunization at the age of 6, 10, and 14 weeks or 8, 12, and 16 weeks using a combined vaccine. To accelerate the introduction of the hepatitis B birth dose vaccine (HepB-BD) into sub-Saharan Africa, it is critical to establish to what extent the addition of HepB-BD can further reduce HBV transmission in areas where three-dose infant vaccination has been implemented. We therefore designed a study to evaluate the impact, acceptability, and cost-effectiveness of incorporating the HepB-BD into the routine immunization program in a real-life field condition in Burkina Faso, where the hepatitis B vaccination is currently scheduled at 8-12-16 weeks. Through a multidisciplinary approach combining epidemiology, anthropology, and health economics, the Neonatal Vaccination against Hepatitis B in Africa (NéoVac) study conducts a pragmatic stepped wedge cluster randomized controlled trial in rural areas of the Hauts-Bassins Region. The study was registered in ClinicalTrials.gov (identifier: NCT04029454). A health center is designated as a cluster, and the introduction of HepB-BD will be rolled out sequentially in 24 centers. Following an initial period in which no health center administers HepB-BD, one center will be randomly allocated to incorporate HepB-BD. Then, at a regular interval, another center will be randomized to cross from the control to the intervention period, until all 24 centers integrate HepB-BD. Pregnant women attending antenatal care will be systematically invited to participate. Infants born during the control period will follow the conventional immunization schedule (8-12-16 weeks), while those born in the interventional period will receive HepB-BD in addition to the routine vaccines (0-8-12-16 weeks). The primary outcome, the proportion of hepatitis B surface antigen (HBsAg) positivity in infants aged at 9 months, will be compared between children born before and after HepB-BD introduction. The study will generate data that may assist governments and stakeholders in sub-Saharan Africa to make evidence-based decisions about whether to add HepB-BD into the national immunization programs. MDPI 2021-06-01 /pmc/articles/PMC8227098/ /pubmed/34206058 http://dx.doi.org/10.3390/vaccines9060583 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Tall, Haoua
Adam, Pierrick
Tiendrebeogo, Abdoul Salam Eric
Vincent, Jeanne Perpétue
Schaeffer, Laura
von Platen, Cassandre
Fernandes-Pellerin, Sandrine
Sawadogo, François
Bokoum, Alkadri
Bouda, Ghislain
Ouattara, Seydou
Ouédraogo, Issa
Herrant, Magali
Boucheron, Pauline
Sawadogo, Appolinaire
Betsem, Edouard
Essoh, Alima
Kabore, Lassané
Ouattara, Amariane
Méda, Nicolas
Hien, Hervé
Gosset, Andréa
Giles-Vernick, Tamara
Boyer, Sylvie
Kania, Dramane
Vray, Muriel
Shimakawa, Yusuke
Impact of Introducing Hepatitis B Birth Dose Vaccines into the Infant Immunization Program in Burkina Faso: Study Protocol for a Stepped Wedge Cluster Randomized Trial (NéoVac Study)
title Impact of Introducing Hepatitis B Birth Dose Vaccines into the Infant Immunization Program in Burkina Faso: Study Protocol for a Stepped Wedge Cluster Randomized Trial (NéoVac Study)
title_full Impact of Introducing Hepatitis B Birth Dose Vaccines into the Infant Immunization Program in Burkina Faso: Study Protocol for a Stepped Wedge Cluster Randomized Trial (NéoVac Study)
title_fullStr Impact of Introducing Hepatitis B Birth Dose Vaccines into the Infant Immunization Program in Burkina Faso: Study Protocol for a Stepped Wedge Cluster Randomized Trial (NéoVac Study)
title_full_unstemmed Impact of Introducing Hepatitis B Birth Dose Vaccines into the Infant Immunization Program in Burkina Faso: Study Protocol for a Stepped Wedge Cluster Randomized Trial (NéoVac Study)
title_short Impact of Introducing Hepatitis B Birth Dose Vaccines into the Infant Immunization Program in Burkina Faso: Study Protocol for a Stepped Wedge Cluster Randomized Trial (NéoVac Study)
title_sort impact of introducing hepatitis b birth dose vaccines into the infant immunization program in burkina faso: study protocol for a stepped wedge cluster randomized trial (néovac study)
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8227098/
https://www.ncbi.nlm.nih.gov/pubmed/34206058
http://dx.doi.org/10.3390/vaccines9060583
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