Progress Toward Elimination of Mother-to-Child Transmission of Hepatitis B Virus — Region of the Americas, 2012–2022

Mary M. Alleman, PhD1; Leandro Soares Sereno, MD2; Alvaro Whittembury, MD3; Xi Li, MD1; Marcela Contreras, MPH3; Carmelita Pacis-Tirso3; Martha Velandia Gonzalez, MD3; Karen Broome, MPH4; Sandra Jones, MPP5; Daniel Salas, MD3; Monica Alonso, PhD2; Rania A. Tohme, MD6; Annemarie Wasley, ScD1 (View author affiliations)

View suggested citation

Summary

What is already known about this topic?

In 2022, 5 million persons in the World Health Organization Region of the Americas (AMR) had chronic hepatitis B virus (HBV) infection, the leading cause of hepatocellular carcinoma and cirrhosis. Hepatitis B birth dose (HepB-BD) vaccination followed by 2–3 additional doses (HepB3) during infancy can prevent chronic infection.

What is added by this report?

All 51 AMR countries provide HepB3; 67% also provide HepB-BD. Mathematical models suggest that hepatitis B prevalence among children has met the global and regional impact target of ≤0.1% in 14 countries and regionally. HepB3 coverage decreased by ≥10 percentage points in 2022 compared with 2012 in 15 countries; 17 countries do not yet provide HepB-BD.

What are the implications for public health practice?

Declines in HepB3 coverage and the absence of HepB-BD in 17 countries’ routine immunization schedules threaten the elimination of mother-to-child transmission of HBV infection throughout AMR. Efforts to introduce HepB-BD and maintain high HepB3 and HepB-BD coverage are needed.

Article Metrics
Altmetric:

Related Materials

Abstract

In 2022, an estimated 5 million persons in the World Health Organization Region of the Americas (AMR) were living with chronic hepatitis B virus (HBV) infection, the leading cause of hepatocellular carcinoma and cirrhosis worldwide. Most chronic infections are acquired through mother-to-child transmission (MTCT) or horizontal transmission during childhood and are preventable with hepatitis B vaccination, including a birth dose (HepB-BD), followed by 2–3 additional doses (HepB3) in infancy. The Pan American Health Organization (PAHO) Elimination of MTCT of HBV infection strategy is intended to reduce chronic HBV infection (measured by hepatitis B surface antigen [HBsAg] seroprevalence) to ≤0.1% among children by achieving 1) ≥95% coverage with HepB-BD and HepB3; and 2) ≥80% of pregnant women received testing for HBsAg, and provision of hepatitis B immunoglobulin to HBV-exposed neonates. By 2012, all 51 AMR countries and territories (countries) provided HepB3 nationwide, and by 2021, 34 (67%) provided HepB-BD nationwide. Mathematical models estimate that HBsAg seroprevalence in children is ≤0.1% in 14 (28%) of 51 countries and at the regional level. Three (6%) of 51 countries met the 95% coverage targets for both HepB3 and HepB-BD during both 2021 and 2022. Of these, two have likely met criteria for the elimination of MTCT of HBV infection. However, in 2022, HepB3 coverage had declined by ≥10 percentage points in 15 (37%) of 41 countries with 2012 coverage data for comparison. These declines in HepB3 coverage, as well as the absence of HepB-BD in the routine immunization schedules in 17 countries, threaten PAHO’s progress toward the elimination of MTCT of HBV infection. Efforts to introduce HepB-BD and maintain high HepB3 and HepB-BD coverage are needed.

Introduction

Globally, chronic hepatitis B virus (HBV) infection is the leading cause of hepatocellular carcinoma and cirrhosis (1). In 2022, an estimated 5 million persons in the World Health Organization (WHO) Region of the Americas (AMR)* had chronic HBV infection, and approximately 20,000 died from hepatitis B–related causes (2). Most chronic HBV infections are acquired through mother-to-child transmission (MTCT) or horizontal transmission during early childhood (1). Infections acquired at age ≤5 years are more likely to become chronic than are those acquired later in life (1). To prevent chronic HBV infection, WHO recommends that all infants receive a timely birth dose of hepatitis B vaccine (HepB-BD), defined as receipt within the first 24 hours of life, with 2–3 additional doses (HepB3) preferably administered during the first months of life, simultaneous with vaccines containing diphtheria, tetanus, and pertussis (1).

In 1999, the Pan American Health Organization (PAHO) recommended that the 51 countries and territories (countries) in AMR provide HepB3 vaccination for all infants nationwide (universal vaccination) and, in 2011, recommended the inclusion of a universal HepB-BD (3,4). In 2017, PAHO expanded its strategy for achieving the elimination of MTCT of HIV and syphilis to include HBV infection and Chagas disease (EMTCT Plus) (5). PAHO’s EMTCT Plus strategy includes the impact target of reducing hepatitis B surface antigen (HBsAg) seroprevalence (a marker for chronic HBV infection) to ≤0.1% among children aged 4–6 years, and several programmatic targets: 1) achieving high coverage (≥95% nationally and >85% in all provinces or areas) with timely HepB-BD and HepB3; and 2) increasing HBsAg testing among pregnant women and provision of hepatitis B immunoglobulin (HBIG) to HBV-exposed neonates to ≥80% (5). The WHO global criteria for the elimination of MTCT of HBV infection are similar and include achieving ≤0.1% HBsAg seroprevalence among children aged ≤5 years and ≥90% coverage with timely HepB-BD and HepB3 for the two most recent, consecutive years (6). This report describes progress toward the elimination of MTCT of HBV infection in AMR during 2012–2022 (3,5,6).

Methods

Vaccination Activities

Hepatitis immunization schedules, year of hepatitis vaccine introduction nationwide (universal), and WHO/UNICEF National Immunization Coverage estimates or administrative immunization coverage for timely HepB-BD and HepB3 among children aged <1 year were compiled from PAHO, UNICEF, and WHO immunization data portals, unless otherwise indicated (3). WHO/UNICEF National Immunization Coverage estimates are based upon annual country reports submitted via the WHO/UNICEF Joint Reporting Form on Vaccination and coverage surveys.

HBsAg Seroprevalence

WHO recommends population-based, nationally representative HBsAg serosurveys among children aged ≤5 years to monitor progress toward the elimination of MTCT of HBV infection (6). Examples of representative serosurveys (national or subnational) in children or cohorts born after introduction and widespread use of hepatitis B vaccine in the AMR were identified through a search of literature published after 2016 and were reviewed (3). Mathematical modeling estimates of HBsAg seroprevalence in children published by the Global Burden of Disease Collaborators,§ The Global Health Observatory, and the Center for Disease Analysis/Polaris Observatory Collaborators** were reviewed and compiled.

Additional Indicators for EMTCT Plus

Data on the proportion of pregnant women with at least four prenatal care visits and of births at health facilities were compiled from PAHO’s Core Indicator Portal. Data describing the presence of policies for universal testing for HBV in antenatal care and provision of HBIG to HBV-exposed newborns were compiled from published literature and PAHO and country websites describing strategies for hepatitis B control and the elimination of MTCT of HBV infection. This activity was reviewed by CDC, deemed not research, and was conducted consistent with applicable federal law and CDC policy.††

Results

Vaccination Activities

HepB3. By 2012, all 51 AMR countries provided universal HepB3 vaccination (3) (Table 1). Regional HepB3 coverage increased steadily during the 1990s and ranged from 88% to 91% during 2005–2016 (Figure) (3). Regional coverage declined to 79% in 2019 but rebounded to 83% in 2022.

HepB3 coverage in 2022 declined by ≥13 percentage points from that in 2012 in the Andean Area, Central America, and Southern Cone and Brazil subregions (Table 1) and declined by ≥10 percentage points in 15 (37%) of 41 countries reporting data for both 2012 and 2022 (3). Coverage in Haiti and Suriname never exceeded 68% and 81%, respectively, during the reporting period. Twelve countries met the global target of ≥90% HepB3 coverage during both 2021 and 2022; among those, five met the PAHO target of ≥95% coverage.

HepB-BD. As of 2021, 34 (67%) countries provided universal HepB-BD vaccination (Table 1) (3). During 2000–2022, regional HepB-BD coverage increased from 23% to 65% (Figure) (3) and during 2012–2022, remained relatively stable or increased in all subregions. Among 15 countries reporting HepB-BD coverage for 2012 and 2022, coverage declined in 2022 by ≥10 percentage points in Argentina, Costa Rica, Mexico, and Venezuela compared with that in 2012 (3). Seven countries met the global target of ≥90% HepB-BD coverage during both 2021 and 2022; among those countries, five met the PAHO target of ≥95% coverage.

HBsAg Seroprevalence

Estimates from three mathematical models suggest that regional HBsAg seroprevalence among children aged ≤5 years is <0.1% (Table 2). Among 26 countries for which three modeled estimates are available, the estimated seroprevalence from all three models is ≤0.1% in 14 (54%) countries, among which two (Chile and Cuba) reported both HepB3 and HepB-BD coverage ≥95% during both 2021 and 2022. Recently published nationally representative HBsAg serosurveys that included children and vaccine-eligible cohorts conducted in Haiti, Mexico, and the United States corroborate the 2022 estimates for these countries. In addition, recently published HBsAg serosurvey results from population-based subnational surveys conducted in AMR show that decades of vaccination against HBV have led to reductions in the seroprevalence of HBsAg among cohorts that have been age-eligible for vaccination compared with seroprevalence among older cohorts.

Additional Indicators for EMTCT Plus

According to reports received by PAHO from 35 countries, as of 2020, 19 (54%) had national goals for the elimination of MTCT of HBV infection (5). Forty-three countries reported data on prenatal care visits by pregnant women; in 21 (49%) countries, ≥90% of pregnant women had at least four prenatal visits. In 27 of 30 (90%) countries with data on delivery location, ≥91.5% of births were at health facilities. Twenty-seven (84%) of 32 countries with data reported providing universal antenatal HBV testing, and 24 (75%) of 32 reported providing HBIG for neonates born to mothers with high levels of HBV DNA; however, the extent of coverage with these interventions is unknown in many AMR countries.

Discussion

Substantial progress has been made toward the elimination of MTCT of HBV infection in AMR. PAHO has supported vaccination against hepatitis B in the region since the 1990s by 1) advocating for vaccination to stakeholders, 2) providing technical support for the development of national vaccination policies, 3) building health care worker capacity, and 4) facilitating vaccine procurement.§§ Mathematical models estimate the prevalence of chronic HBV infection among children aged ≤5 years, as measured by HBsAg seroprevalence, to be <0.1% regionally, and 14 countries met both regional and global impact targets for the elimination of MTCT of HBV infection (5,6). Among the 14 countries identified as likely to have met the HBsAg seroprevalence target, two reported HepB-BD and HepB3 coverage ≥95% during both 2021 and 2022, meeting both the regional and global programmatic targets for the elimination of MTCT of HBV infection, and both implemented antenatal and maternal and child health policies supporting the elimination of MTCT of HBV infection (5,6).

PAHO has endorsed a process for validating achievement of the elimination of MTCT of HBV infection (6), and regional and national validation committees have been established. Because countries are evaluated for the elimination of MTCT of HBV infection, representative seroprevalence data documenting the prevalence of chronic HBV infection in children are needed. Innovative approaches, such as the integration of HBsAg testing into other surveys or sampling focused on geographic areas with documented high risk for HBV infection such as the two-phase method for verifying the elimination of MTCT of HBV infection used in Colombia (7), might facilitate the collection of essential data.

Despite regional progress, an estimated 34,000 children aged ≤5 years in the Americas had chronic HBV infection in 2022 (8). Few countries are consistently achieving the ≥90% HepB3 global coverage target. Declines in HepB3 coverage during 2012–2022 threaten progress toward elimination of chronic HBV infection in children. These declines have been attributed to inadequate sustainable financing and reductions in social mobilization for vaccination, increasing vaccination hesitancy, insecurity linked to civil unrest, lack of easy access to health services for some populations, and recently, the COVID-19 pandemic and consequent health service disruptions¶¶,***,†††,§§§,¶¶¶ (9,10). To overcome these constraints and improve HepB3 vaccination coverage, PAHO is working with countries to implement the recommendations in the 2021 Reinvigorating Immunization as a Public Good for Universal Health resolution**** and the new Regional Immunization Action Plan 2030.††††

Although most children born in AMR live in countries with routine HepB-BD, 17 countries, particularly in the Caribbean and Latin Caribbean subregions (13 of the 17), have not introduced universal birth dose vaccination (3). In countries with HepB-BD, efforts to address disparities in coverage and access and to ensure timely administration will protect infants at risk for HBV infection (1). Most births in the region occur at health facilities; thus, implementation of policies such as standing orders for newborn HepB-BD vaccination before discharge of mother and child, paired with education of pregnant women and maternal and child health care staff members about the importance of the birth dose, can improve timely administration and coverage.

The region continues to expand efforts to achieve the elimination of MTCT of HBV infection by integrating antenatal viral testing, antiviral treatment during pregnancy when indicated, and provision of HBIG for HBV-exposed newborns into the established platforms providing interventions for the elimination of MTCT of HIV and syphilis (5). PAHO’s Strategic Fund is tasked with improving access to and reducing costs of hepatitis B–relevant health supplies and medicines for the region.§§§§

Limitations

The findings in this report are subject to at least two limitations. First, current HepB-BD and HepB3 vaccination schedules and coverage or the elimination of MTCT programmatic indicators were not available for all countries or all years, limiting the completeness of summaries on regional progress on the elimination of MTCT of HBV infection. Second, not all countries have systems that differentiate reporting of timely versus any HepB-BD administration, thus potentially overestimating timely birth dose coverage.

Implications for Public Health Practice

Although progress has been made, declines in HepB3 coverage and the absence of HepB-BD introduction in 17 countries threaten PAHO’s progress toward the elimination of MTCT of HBV infection. To advance toward the regional goal of the elimination of MTCT of HBV infection, continued efforts are needed to support HepB-BD introduction and the achievement and maintenance of high HepB-BD and HepB3 coverage.

Acknowledgments

Holly A. Hill, David Yankey, Immunization Services Division, National Center for Immunization and Respiratory Diseases, CDC; Jose A. Rodrigues, Epidemiology Elective Program, National Center for State, Tribal, Local, and Territorial Public Health Infrastructure and Workforce, CDC.

Corresponding author: Mary M. Alleman, mea4@cdc.gov.


1Global Immunization Division, Global Health Center, CDC; 2Communicable Disease Prevention, Control and Elimination Department, Pan American Health Organization/WHO Regional Office for the Americas, Washington, DC; 3The Special Program Comprehensive Immunization, Pan American Health Organization/WHO Regional Office for the Americas, Washington, DC; 4The Special Program Comprehensive Immunization, Subregional Program Coordination, Caribbean, Pan American Health Organization/WHO Regional Office for the Americas, Washington, DC; 5Communicable Disease Prevention, Control and Elimination Department, Subregional Program Coordination, Caribbean, Pan American Health Organization/WHO Regional Office for the Americas, Washington, DC; 6Division of Viral Hepatitis, National Center for HIV, Viral Hepatitis, STD, and TB Prevention, CDC.

All authors have completed and submitted the International Committee of Medical Journal Editors form for disclosure of potential conflicts of interest. No potential conflicts of interest were disclosed.


* PAHO/AMR consists of 51 countries and territories (referred to as countries in the text) as follows. Countries (35): Antigua and Barbuda, Argentina, Bahamas, Barbados, Belize, Bolivia, Brazil, Canada, Chile, Colombia, Costa Rica, Cuba, Dominica, Dominican Republic, Ecuador, El Salvador, Grenada, Guatemala, Guyana, Haiti, Honduras, Jamaica, Mexico, Nicaragua, Panama, Paraguay, Peru, St. Lucia, St. Vincent and the Grenadines, St. Kitts and Nevis, Suriname, Trinidad and Tobago, United States, Uruguay, and Venezuela; and territories (16): Anguilla, Aruba, Bermuda, Bonaire, Cayman Islands, Curaçao, French Guiana, Guadeloupe, Martinique, Montserrat, Puerto Rico, Saba, Sint Eustatius, Sint Maarten, Turks and Caicos Islands, and British Virgin Islands.

Globally, WHO has defined the target as ≤0.1% HBsAg seroprevalence in children aged ≤5 years. In countries with a long history of sustained, high hepatitis B vaccination coverage, flexibility exists to conduct surveys among children aged >5 years. In AMR, PAHO has set the target age group for hepatitis B serosurveys to be children aged 4–6 years.

§ https://www.healthdata.org/research-analysis/gbd (Accessed July 2, 2024).

https://www.who.int/data/gho (Accessed July 2, 2024).

** https://cdafound.org/polaris/

†† 45 C.F.R. part 46, 21 C.F.R. part 56; 42 U.S.C. Sect. 241(d); 5 U.S.C. Sect. 552a; 44 U.S.C. Sect. 3501 et seq.

§§ https://www.paho.org/en/revolving-fund

¶¶ https://www.paho.org/en/news/20-4-2023-risk-vaccine-preventable-disease-outbreaks-30-year-high-paho-director-says

*** https://www.unicef.org/lac/en/press-releases/1-in-4-children-in-latin-america-and-caribbean-is-missing-out-life-saving-vaccines

††† https://www.ijidonline.com/article/S1201-9712(19)30143-2/pdf

§§§ https://www.connectas.org/the-silent-backslide-of-childhood-vaccination-in-latin-america/

¶¶¶ https://www.paho.org/en/news/27-7-2021-disruption-health-services-during-covid-19-pandemic-threatens-elimination-hepatitis

**** https://www.paho.org/en/documents/ce16814-reinvigorating-immunization-public-good-universal-health

†††† https://www.paho.org/en/events/webinar-regional-immunization-action-plan-americas-2030

§§§§ https://www.paho.org/en/paho-strategic-fund

References

  1. World Health Organization. Hepatitis B vaccines: WHO position paper—July 2017. Wkly Epidemiol Rec 2017;92:369–92. https://www.who.int/publications/i/item/WER9227 PMID:28685564
  2. World Health Organization. Global hepatitis report 2024: action for access in low- and middle-income countries. Geneva, Switzerland: World Health Organization; 2024. https://www.who.int/publications/i/item/9789240091672
  3. Ropero Álvarez AM, Pérez-Vilar S, Pacis-Tirso C, et al. Progress in vaccination towards hepatitis B control and elimination in the Region of the Americas. BMC Public Health 2017;17:325 https://doi.org/10.1186/s12889-017-4227-6 PMID:28415981
  4. Pan American Health Organization; World Health Organization. 1999–2015 TAG recommendations for hepatitis B: Washington, DC: Pan American Health Organization; World Health Organization Regional Office for the Americas; 2015. https://www.paho.org/en/documents/1999-2015-tag-recommendations-hepatitis-b
  5. Pan American Health Organization; World Health Organization. Elimination of mother-to-child transmission of HIV, syphilis, perinatal hepatitis B, and congenital Chagas disease. Washington, DC: Pan American Health Organization; World Health Organization Regional Office for the Americas; 2017. https://www.paho.org/en/topics/elimination-mother-child-transmission-hiv-syphilis-perinatal-hepatitis-b-and-congenital
  6. World Health Organization. Global guidance on criteria and processes for validation: elimination of mother-to-child transmission of HIV, syphilis, and hepatitis B virus. Geneva, Switzerland: World Health Organization; 2022. https://www.who.int/publications/i/item/9789240039360
  7. Ríos-Hincapié CY, Murad-Rivera R, Tohme RA, et al. Progress towards the elimination of hepatitis B in children in Colombia: a novel two-phase study approach. J Viral Hepat 2022;29:737–47. https://doi.org/10.1111/jvh.13719 PMID:35707957
  8. Polaris Observatory Collaboratorset al. Global prevalence, cascade of care, and prophylaxis coverage of hepatitis B in 2022: a modelling study. Lancet Gastroenterol Hepatol 2023;8:879–907 https://doi.org/10.1016/S2468-1253(23)00197-8 PMID:37517414
  9. Taylor L. Covid-19: PAHO calls for Americas to reverse vaccination setbacks caused by pandemic. BMJ 2022;378:o2344 https://www.bmj.com/content/378/bmj.o2344. https://doi.org/10.1136/bmj.o2344 PMID:36170992
  10. Castro-Aguirre IE, Alvarez D, Contreras M, et al. The impact of the coronavirus pandemic on vaccination coverage in Latin America and the Caribbean. Vaccines (Basel) 2024;12:458. https://doi.org/10.3390/vaccines12050458 PMID:38793709
TABLE 1. Year of introduction of hepatitis B vaccine,*, hepatitis B vaccination schedules,§, and annual estimated or official coverage with third dose of hepatitis B vaccine and a timely hepatitis B birth dose**,††,§§ among children aged <1 year, by country or territory, subregion, and region — Region of the Americas, World Health Organization, 2012, 2017, and 2019–2022Return to your place in the text
Subregion, Country/Territory¶¶ Year of introduction HepB vaccination schedule HepB3 coverage, % Timely HepB-BD coverage, %
HepB3 HepB-BD 2012 2017 2019 2020 2021 2022 2012 2017 2019 2020 2021 2022
North America** NA NA NA 92 78 79 86 88 89 43 37 41 59 60 62
Canada 1993 1983 Varies by province§ 70 71 84 84 84 83 NR NR NR NR NR NR
Mexico 1999 2007 B, 2, 4, and 6 mos 99 58 56 77 80 83 94§§ NR NR 50 50 50
United States 1991 1991 B,1–2, and 6–18 mos§ 90 91 91 91 92 93 72 63 67 69 72 75
Central America** NA NA NA 95 91 89 83 81 82 43 60 58 57 55 54
Costa Rica 1997 1997 B, 2, and 6 mos 91 97 94 91 87 94 90 87 87 89 71 71
El Salvador 1999 2015 B, 2, 4, and 6 mos 92 92 90 76 78 75 NA 91 91 90 87 86
Guatemala 2005 2010 B, 2, 4, and 6 mos 96 91 85 83 79 79 35 53 48 48 48 48
Honduras 2000 2007 B, 2, 4, and 6 mos 98 90 88 80 77 78 78 78 78 71 72 69
Nicaragua 1999 NA 2, 4, and 6 mos 98 98 98 92 87 92 NA NA NA NA NA NA
Panama 1999 2002 B, 2, 4, and 6 mos 85 81 88 74 87 87 87 87 85 86 87 87
Andean Area** NA NA NA 90 84 83 73 75 76 62 65 67 65 62 62
Bolivia 2000 NA 2, 4, and 6 mos 93 84 75 68 70 69 NA NA NA NA NA NA
Colombia†† 1994 2001 B, 2, 4, and 6 mos 92 92 92 88 86 87 85 81 81 88 87 85
Ecuador 1999 2009 B, 2, 4, and 6 mos 88 85 85 70 68 70 16 61 71 62 61 63
Peru 2003 2003 B, 2, 4, and 6 mos 95 89 88 72 82 82 81 80 82 75 77 79
Venezuela 2000 2008 B, 2, 4, and 6 mos 81 66 64 54 56 56 67 56 52 50 37 37
Southern Cone and Brazil** NA NA NA 95 84 76 78 72 79 80 74 73 64 64 78
Argentina 2000 2000 B, 2, 4, and 6 mos 91 86 83 74 81 81 88 80 77 72 77 77
Brazil 1998 1998 B, 2, 4, and 6 mos 96 82 72 77 68 77 90 80 77 63 62 82
Chile 2005 2019 B, 2, 4, and 6 mos 90 93 96 93 95 96 NA NA 65 99 98 99
Paraguay†† 2002 2017 B, 2, 4, and 6 mos 91 91 86 79 70 69 NA 52 NR NR NR NR
Uruguay 1999 NA 2, 4, and 6 mos 95 93 94 92 91 94 NA NA NA NA NA NA
Latin Caribbean** NA NA NA 46 77 72 71 71 72 47 49 47 44 42 43
Cuba 1990 1992 B, 2, 4, and 6 mos 96 99 99 99 99 99 99 99 99 99 99 99
Dominican Republic 1994 1997 B, 2, 4, and 6 mos 74 81 87 81 83 87 74 82 81 71 66 71
French Guiana 1994 2008 B, 2, and 11 mos NR NR NR NR NR NR NR NR NR NR NR NR
Guadeloupe NR NR 2, 4, and 11 mos NR NR NR NR NR NR NR NR NR NR NR NR
Haiti 2012 NA 6, 10, and 14 wks NR 64 51 51 51 51 NA NA NA NA NA NA
Martinique NR NR 2, 4, and 11 mos NR NR NR NR NR NR NR NR NR NR NR NR
Puerto Rico 1994 1999 B, 1–2, and 6–18 mos§ NA NA 73 NA NA NA NA NA 59 NA NA NA
The Caribbean** NA NA NA 92 90 93 86 86 90 5 9 22 24 29 30
Anguilla†† 1997 2019 B, 2, 4, and 6 mos 100§§ 89 77 86 79 88 NA NA 100 100 100 100
Antigua and Barbuda 2000 2021 B, 2, 4, and 6 mos 98 95 99 95 92 99 NA NA NA NA 19 19
Aruba†† 2003 NA 1, 3, and 9 mos 94§§ 95 94 NR 92 93 NA NA NA NA NA NA
Bahamas 2001 NA 2, 4, and 6 mos 96 94 89 83 86 87 NA NA NA NA NA NA
Barbados 2001 NA 2, 4, and 6 mos 87 90 90 85 82 86 NA NA NA NA NA NA
Belize 1999 2018 B, 2, 4, and 6 mos 98 88 98 79 83 84 NA NA 70 67 77 86
Bermuda†† 1997 NA 6, 7, and 12 mos 92§§ 81 97 89 100 89 NA NA NA NA NA NA
Bonaire 2012 NR 2 mos, 14 wks, 5 mos, and 11 mos NR NR NR NR NR NR NR NR NR NR NR NR
Cayman Islands†† 1997 1997 B, 6 wks, and 9 mos 94§§ 87 NR 79 84 90 NR NR NR 75 NR NR
Curaçao†† 2011 NR B, 8, 14, and 22 wks NR 85 98 NR NR NR NR NR NR NR NR NR
Dominica 2006 2017 B, 2, 4, and 6 mos 97 91 99 97 92 92 NA 23 97 99 98 99
Grenada 2001 2017 B, 6–8, 16, and 24 wks 97 96 94 72 77 77 NA 78 96 92 90 91
Guyana 2001 2019 B, 2, 4, and 6 mos 97 97 99 99 98 98 NA NA 35 49 58 57
Jamaica 2003 NA 6, 12, and 24 wks 96 93 96 95 89 98 NA NA NA NA NA NA
Montserrat†† 1999 2017 B, 2, 4, and 6 mos 94§§ 100 100 NR NR 98 NA 100 100 NR 80 83
Saba 2012 NR 2, 3, 4, and 11 mos 100§§ NR NR NR NR NR NR NR NR NR NR NR
Saint Kitts and Nevis 1999 2015 B, 2, 4, and 6 mos 98 98 97 99 96 96 NA 83 84 93 95 96
Saint Lucia 2002 2018 B, 2, 4, and 6 mos 98 80 92 86 80 81 NA NA 85 86 94 82
Saint Vincent and the Grenadines 2003 2017 B, 2, 4, and 6 mos 96 99 98 98 99 99 NA 30 99 96 93 93
Sint Eustatius 1997 NR 2, 3, 4, and 11 mos NR NR NR NR NR NR NR NR NR NR NR NR
Sint Maarten†† 2000 NA 2, 3, and 6 mos 91§§ 94 NR NR NR NR NA NA NA NA NA NA
Suriname 2005 2005 B, 2, 4, and 6 mos 76 67 77 51 72 77 51 80 79 79 79 79
Trinidad and Tobago 2003 NA 2, 4, and 6 mos 92 89 93 96 94 93 NA NA NA NA NA NA
Turks and Caicos Islands†† 1999 2019 B, 2, 4, and 6 mos 95§§ 93 93 84 92 99 NA NA NR NR NR 100
British Virgin Islands†† 1999 2016 B, 2, 4, and 6 mos 97§§ 82 88 87 84 100 NA 90 98 94 NR 91
Total for Region of the Americas** NA NA NA 91 82 79 81 80 83 56 54 55 60 60 65

Abbreviations: B = at birth; HepB = hepatitis B–containing vaccine; HepB3 = third dose of HepB; HepB-BD = birth dose of HepB; JRF = World Health Organization/UNICEF Joint Reporting Form on Vaccination; NA = not applicable; NR = data not reported; WUENIC = World Health Organization/UNICEF estimates of national immunization coverage.
* Year of introduction refers to the year the country or territory established universal HepB vaccination (HepB3 or HepB-BD) policies (i.e., HepB vaccination is recommended for all children throughout the country or territory according to schedule).
All years of HepB3 introduction and all years of HepB-BD introduction before 2016 were compiled from https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5392937. Years of HepB-BD introduction during and after 2016 were compiled from https://data.unicef.org/resources/immunization-country-profiles, https://paho-cim.shinyapps.io/immunization-dashboard, https://immunizationdata.who.int/global/wiise-detail-page/introduction-of-hepb-birth-dose?ISO_3_CODE = PRY&YEAR =, or directly from the JRF.
§ HepB vaccination schedules were compiled from https://immunizationdata.who.int/. Canada’s provinces have varying schedules; some include a birth dose, and some initiate vaccination after 1 year of life. Details by Canadian province are available online (https://www.canada.ca/en/public-health/services/provincial-territorial-immunization-information.html). For the United States (including Puerto Rico), the HepB vaccination schedule was extracted from https://www.cdc.gov/vaccines/schedules/downloads/child/0-18yrs-child-combined-schedule.pdf.
If not available at https://immunizationdata.who.int/ or as indicated in footnote above, HepB vaccination schedules were compiled from https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5392937.
** Annual HepB3 and HepB-BD national coverage values are WUENIC prepared using data from the JRF; they were compiled from https://immunizationdata.who.int. Timely administration of HepB-BD is defined as administration within 24 hours of birth. For the United States, coverage estimates were determined as follows for HepB3 and HepB-BD: 2016–2018 estimates are among children aged 19–35 months during the previous survey year (e.g., 2018 estimate is from survey year 2017 data); 2019–2022 estimates are among children by age 24 months. The 2019 estimate is from combined 2015–2016 birth cohort, the 2020 estimate is from combined 2016–2017 birth cohort, the 2021 estimate is from combined 2017–2018 birth cohort, and the 2022 estimate is from combined 2018–2019 birth cohort. For Puerto Rico, HepB3 estimates are among children by age 24 months, by birth cohort; HepB-BD estimates are among children on the first day of life, by birth cohort. Data were not collected in Puerto Rico during some of the reporting years. In addition, even when data were collected, sample size was sometimes too small to calculate reliable coverage estimates. HepB3 and HepB-BD subregional and regional coverage estimates were generated using data from the 10-year period (2012–2022) for the 51 countries or territories using WUENIC estimates or official coverage. Countries or territories not reporting coverage or that have not adopted universal HepB-BD vaccination policies were assumed to have no coverage. HepB3 and HepB-BD subregional and regional coverage values were weighted coverage based upon the number of average annual births for 2012–2022, as available, from the United Nations population estimates.
†† Where annual WUENIC were not available, values are from official or administrative national immunization coverage as reported on the country or territory’s JRF (https://paho-cim.shinyapps.io/immunization-dashboard). Any reported coverage exceeding 100% was considered 100%.
§§ Where annual WUENIC and official or administrative national immunization coverage as reported on the country or territory’s JRF were not available, values are those provided in a previous report. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5392937
¶¶ Vaccination data for some territories within the Region of the Americas are not consistently reported to the World Health Organization separately from their associated countries.

Return to your place in the textFIGURE. Annual estimated coverage with the third dose of hepatitis B vaccine and timely hepatitis B birth dose* among children aged <1 year — Region of the Americas, World Health Organization, 1993–2022
The figure is a line chart showing annual estimated regional coverage with the third dose of hepatitis B vaccine and timely hepatitis B birth dose among children aged <1 year in the World Health Organization Region of the Americas during 1993–2022.

Abbreviations: HepB3 = third dose of hepatitis B–containing vaccine; HepB-BD = birth dose of hepatitis B monovalent vaccine; WHO = World Health Organization.

* Regional coverage values are based upon WHO/UNICEF National Immunization Coverage estimates and were compiled from the WHO immunization data portal. https://immunizationdata.who.int

TABLE 2. Estimated hepatitis B surface antigen seroprevalence among children aged <5 years, coverage of reproductive health and maternal and child health services, and policies of interventions for the prevention of mother-to-child transmission of hepatitis B, by country or territory and region — Region of the Americas, World Health Organization, 2008–2022Return to your place in the text
Subregion, Country/Territory Estimated HBsAg seroprevalence among children aged ≤5 years, % (95% CI)* Estimated antenatal care coverage with ≥4 visits, %
(yr of data)**
Estimated births at health facilities, %
(yr of data)**
Policy
Global Burden of Disease collaborators, 2019 The Global Health Observatory,§ 2020 Center for Disease Analysis/Polaris Observatory collaborators, 2022 Universal HBV testing in antenatal care, 2020–2022†† Provision of HBIG to HBV-exposed newborns,
2020§§
North America
Canada¶¶ 0.3 (0.2–0.3) 0.34 (0.29–0.39) <0.1 (<0.1–<0.1) 99.0 (2020) NR Yes Yes
Mexico*** 0.02 (0.01–0.02) 0.03 (0.02–0.04) <0.1 (<0.1–<0.1) 89.6 (2022) NR NR Yes
United States*** 0.03 (0.02–0.04) 0.01 (0.01–0.02) <0.1 (<0.1–<0.1) 95.4 (2021) 97.8 (2021) Yes Yes
Central America
Costa Rica 0.02 (0.02–0.03) 0.02 (0.01–0.03) <0.1 (<0.1–<0.1) 94.1 (2022) 98.9 (2022) Yes Yes
El Salvador 0.07 (0.05–0.10) 0.02 (0.01–0.07) <0.1 (<0.1–<0.1) 87.2 (2021) 99.7 (2022) No No
Guatemala 0.2 (0.1–0.2) 0.03 (0.02–0.04) <0.1 (<0.1–<0.1) 43.0 (2014) 71.0 (2021) Yes No
Honduras 0.1 (0.1–0.2) 0.03 (0.01–0.11) <0.1 (<0.1–<0.1) 89.0 (2012) 61.4 (2022) No No
Nicaragua 0.03 (0.03–0.03) 0.09 (0.05–0.17) <0.1 (<0.1–0.1) 91.9 (2022) 96.3 (2022) NR NR
Panama 0.08 (0.05–0.11) 0.07 (0.05–0.09) <0.1 (<0.1–<0.1) 88.2 (2019) 91.5 (2021) Yes No
Andean Area
Bolivia 0.03 (0.02–0.04) 0.14 (0.05–0.29) <0.1 (<0.1–<0.1) 81.3 (2022) 93.1 (2022) NR NR
Colombia¶¶ 0.3 (0.2–0.3) 0.15 (0.12–0.19) <0.1 (<0.1–<0.1) 81.6 (2021) 97.3 (2021) Yes Yes
Ecuador 0.04 (0.03–0.06) 0.09 (0.03–0.33) <0.1 (<0.1–0.1) 79.0 (2013) 96.0 (2020) Yes Yes
Peru¶¶ 0.04 (0.03–0.05) 0.06 (0.05–0.07) <0.1 (<0.1–<0.1) 85.1 (2022) 93.3 (2022) Yes Yes
Venezuela 0.1 (0.1–0.2) 0.15 [0.12–0.18] 0.2 (0.2–0.4) 82.6 (2018) NR No Yes
Southern Cone and Brazil
Argentina 0.02 (0.01–0.03) 0.01 (0.01–0.02) <0.1 (<0.1–<0.1) 72.8 (2021) 97.8 (2021) Yes Yes
Brazil 0.1 (0.1–0.2) 0.03 (0.02–0.03) <0.1 (<0.1–<0.1) 92.9 (2022) 98.9 (2021) Yes Yes
Chile 0.02 (0.01–0.03) 0.03 (0.02–0.05) <0.1 (<0.1–<0.1) NR 99.6 (2021) Yes Yes
Paraguay 0.1 (0.1–0.2) 0.42 (0.09–2.08) <0.1 (<0.1–<0.1) 79.6 (2021) NR Yes Yes
Uruguay 0.01 (0.01–0.02) 0.15 (0.02–1.21) NA 97.2 (2022) 100.0 (2021) Yes Yes
Latin Caribbean
Cuba 0.02 (0.02–0.03) 0.03 (0.01–0.05) <0.1 (<0.1–<0.1) 79.3 (2019) 99.8 (2022) Yes Yes
Dominican Republic 0.2 (0.1–0.2) 0.1 (0.03–0.37) 0.1 (<0.1–0.1) 92.6 (2019) 99.9 (2021) NR NR
French Guiana NA NA NA 84.5 (2016) NR NR NR
Guadeloupe NA NA NA NR NR NR NR
Haiti*** 0.3 (0.2–0.4) 1.04 (0.75–1.41) 0.4 (0.3–0.8) 67.0 (2012) 67.3 (2021) No No
Martinique NA NA NA 98.5 (2016) NR NR NR
Puerto Rico 0.04 (0.03–0.05) NA NA 97.8 (2020) 98.8 (2020) NR NR
The Caribbean
Anguilla NA NA NA 100.0 (2012) 100.0 (2022) Yes Yes
Antigua and Barbuda 0.03 (0.02–0.04) 0.19 (0.07–0.68) NA 75.0 (2022) 99.0 (2022) Yes Yes
Aruba NA NA NA 100.0 (2020) NR NR NR
Bahamas 0.03 (0.02–0.04) 0.16 (0.01–4.56) NA 81.2 (2019) 99.2 (2022) Yes Yes
Barbados 0.03 (0.02–0.05) 0.18 (0.05–0.55) NA 90.0 (2020) 98.2 (2022) Yes No
Belize 0.07 (0.05–0.09) 0.6 (0.46–0.76) <0.1 (<0.1–<0.1) NR 92.1 (2022) Yes No
Bermuda 0.2 (0.2–0.3) NA NA 98.0 (2021) 99.8 (2021) Yes Yes
Bonaire NA NA NA NR NR NR NR
Cayman Islands NA NA NA 97.0 (2017) NR Yes Yes
Curaçao NA NA NA NR NR NR NR
Dominica 0.04 (0.02–0.05) 0.2 (0.06–0.6) NA 95.0 (2020) 99.0 (2022) Yes Yes
Grenada 0.06 (0.04–0.08) 0.12 (0.04–0.42) NA 69.0 (2021) NR Yes Yes
Guyana 0.05 (0.03–0.07) 0.4 (0.07–2.11) 0.1 (<0.1–0.2) 95.0 (2022) NR Yes No
Jamaica 0.01 (0.01–0.02) 0.55 (0.37–0.79) 0.2 (0.1–0.3) 87.0 (2008) NR No Yes
Montserrat NA NA NA 100.0 (2022) NR NR NR
Saba NA NA NA NR NR NR NR
Saint Kitts and Nevis 0.03 (0.02–0.04) 0.06 (0.02–0.22) NA 85.0 (2022) 100.0 (2022) NR NR
Saint Lucia 0.05 (0.04–0.07) 0.22 (0.06–0.77) NA 90.0 (2022) 99.0 (2022) NR NR
Saint Vincent and the Grenadines 0.02 (0.01–0.03) 0.15 (0.05–0.49) NA NR NR NR NR
Sint Eustatius NA NA NA NR NR NR NR
Sint Maarten NA NA NA 100.0 (2018) NR NR NR
Suriname 0.04 (0.03–0.05) 0.07 (0.02–0.28) 0.1 (0.1–0.2) 66.8 (2010) NR Yes Yes
Trinidad and Tobago 0.06 (0.04–0.08) 0.19 (0.04–0.81) 0.1 (0.1–0.2) 100.0 (2017) NR NR NR
Turks and Caicos Islands NA NA NA 57.7 (2022) 100.0 (2022) Yes Yes
British Virgin Islands 0.1 (0.1–0.1) NA NA 100.0 (2017) 100.0 (2022) Yes NR
Region of the Americas 0.08 (0.060.11) 0.07 (0.050.13) <0.1 (<0.1<0.1)

Abbreviations: HBIG = hepatitis B immune globulin; HBsAg = hepatitis B surface antigen; HBV = hepatitis B virus; NA = not available; NR = not reported.
* Data are presented in the format of original publication from referenced sources; thus, formatting within and between columns might differ.
https://www.thelancet.com/journals/langas/article/PIIS2468-1253(22)00124-8/fulltext
§ https://www.who.int/data/gho/data/indicators/indicator-details/GHO/hepatitis-b-surface-antigen-(hbsag)-prevalence-among-children-under-5-years
https://cdafound.org/polaris-countries-database/; https://www.sciencedirect.com/science/article/abs/pii/S2468125323001978?via%3Dihub
** https://opendata.paho.org/en/core-indicators/core-indicators-dashboard
†† Universal testing for HBV in antenatal care is the HBsAg testing of all women seeking antenatal care for the purposes of determining their eligibility for antiviral treatment during pregnancy and for the provision of HBIG to the exposed newborn (https://www.who.int/publications/i/item/9789240090903 [Accessed May 9, 2024]). Data are from Towards the Elimination of HIV, Syphilis, Hepatitis B, and Chagas disease in the Americas, EMTCT Plus Initiative 2010–2021, Annex Tables 1 and 4 (https://www.paho.org/en/documents/fact-sheet-emtct-plus-initiative-2011-2021-towards-elimination-hiv-syphilis-hepatitis-b); https://www.canada.ca/en/public-health/services/publications/healthy-living/canadian-immunization-guide-part-4-active-vaccines/page-7-hepatitis-b-vaccine.html; https://www.sciencedirect.com/science/article/pii/S0749379723000569?via%3Dihub; https://www.cdc.gov/hepatitis/statistics/2022surveillance/perinatal-hepatitis-b.htm [All accessed May 24, 2024].
§§ HBIG prophylaxis provided within 24 hours of birth, in conjunction with hepatitis B birth dose vaccination, might be of additional benefit for infants whose mothers are HBsAg-positive, particularly if they have high levels of HBV DNA (https://www.who.int/publications/i/item/9789240090903). Data are from Towards the Elimination of HIV, Syphilis, Hepatitis B, and Chagas disease in the Americas, EMTCT Plus Initiative 2010–2021, Annex Tables 1 and 4 (https://www.paho.org/en/documents/fact-sheet-emtct-plus-initiative-2011-2021-towards-elimination-hiv-syphilis-hepatitis-b) or through direct consultation with countries in 2020.
¶¶ Subnational HBsAg serosurveys targeting high-risk areas that enrolled representative samples of children or vaccine-eligible cohorts illustrate the impact of vaccination against hepatitis B are as follows. Canada: https://pubmed.ncbi.nlm.nih.gov/28736196; Colombia: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10200037; https://www.sciencedirect.com/science/article/pii/S0264410X17315463?via%3Dihub; https://pubmed.ncbi.nlm.nih.gov/28780978/; and Peru: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7410281/pdf/pone.0236993.pdf; https://rpmesp.ins.gob.pe/index.php/rpmesp/article/view/4696/3681; https://www.medigraphic.com/pdfs/salpubmex/sal-2020/sal203b.pdf
*** Nationally representative HBsAg serosurveys are as follows. Haiti: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6609174; Mexico: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6422518/pdf/khvi-15-02-1533617.pdf; and the United States: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10069827; https://pubmed.ncbi.nlm.nih.gov/26251317


Suggested citation for this article: Alleman MM, Sereno LS, Whittembury A, et al. Progress Toward Elimination of Mother-to-Child Transmission of Hepatitis B Virus — Region of the Americas, 2012–2022. MMWR Morb Mortal Wkly Rep 2024;73:648–655. DOI: http://dx.doi.org/10.15585/mmwr.mm7329a3.

MMWR and Morbidity and Mortality Weekly Report are service marks of the U.S. Department of Health and Human Services.
Use of trade names and commercial sources is for identification only and does not imply endorsement by the U.S. Department of Health and Human Services.
References to non-CDC sites on the Internet are provided as a service to MMWR readers and do not constitute or imply endorsement of these organizations or their programs by CDC or the U.S. Department of Health and Human Services. CDC is not responsible for the content of pages found at these sites. URL addresses listed in MMWR were current as of the date of publication.

All HTML versions of MMWR articles are generated from final proofs through an automated process. This conversion might result in character translation or format errors in the HTML version. Users are referred to the electronic PDF version (https://www.cdc.gov/mmwr) and/or the original MMWR paper copy for printable versions of official text, figures, and tables.

Questions or messages regarding errors in formatting should be addressed to mmwrq@cdc.gov.