ACIP Grading of Recommendations Assessment, Development and Evaluation (GRADE) for Hepatitis B (HepB) Vaccine in Adults
Introduction
Since hepatitis B (HepB) vaccine introduction in 1982, there have been substantial declines in reported hepatitis B cases. However, despite reductions in hepatitis B incidence achieved through incremental HepB vaccine policy over the past four decades, from a high of 26,654 reported cases (287,000 estimated) in 1985 to a low of 2,791 reported cases (19,200 estimated) in 2014, progress has stalled in further reducing hepatitis B incidence (1). In 2018, the reported HepB vaccination coverage (≥3 doses) was overall 30.0% for adults ≥19 years old, demonstrating small increases in coverage throughout the past four decades (2), including low coverage among persons in risk groups recommended for vaccination (e.g., 33% coverage among persons with chronic liver disease).
As part of ACIP’s process, a systematic review and Grading of Recommendations Assessment, Development and Evaluation (GRADE) of the evidence of benefits and harms was conducted and presented to ACIP. The GRADE approach for evaluating evidence, which indicates the certainty of estimates from the available body of evidence, was adopted by ACIP in 2010 (3).
Methods
During September 2019–October 2021, the ACIP Hepatitis Work Group held monthly conference calls to review and discuss scientific evidence relevant to the use of HepB vaccines in a universal adult vaccination recommendation. The Work Group identified critical and important outcomes for inclusion in the GRADE tables, conducted a systematic review of the evidence, and subsequently reviewed and discussed findings and evidence quality (www.cdc.gov/vaccines/acip/recs/index.html) (3) (Table 1). In the GRADE approach, evidence certainty can range from type 1 (high certainty) to type 4 (very low certainty). Evidence was found to be available only for the cardiovascular and serious adverse events outcomes. Ultimately, no studies were available comparing the two strategies of universal and risk-based adult HepB vaccination. Thus, only the outcomes of serious adverse events and cardiovascular events associated with Heplisav-B were assessed, as noted below.
- 2019 Viral Hepatitis Surveillance Report. 2021, Centers for Disease Control and Prevention.
- Lu, P.J., et al., Surveillance of Vaccination Coverage Among Adult Populations -United States, 2018. MMWR Surveill Summ, 2021. 70(3): p. 1-26.
- CDC. New Framework (GRADE) for Development of Evidence-Based Recommendations by the Advisory Committee on Immunization Practices. MMWR Recomm Rep 2012;61:327.
Table 1: Policy Question and PICO
| Policy question: | Should all hepatitis B (HepB)-unvaccinated adults receive HepB vaccination? |
|---|---|
| Population | Previously unvaccinated adults age ≥ 18 years |
| Intervention | Universal vaccination strategy (2- and 3-dose schedules) |
| Comparison | Current risk-based vaccination strategy (2- and 3-dose schedules) |
| Outcomes |
|
* This outcome is solely aimed at assessing the 2-dose Heplisav-B vaccine (approved in 2017). The 3-dose HepB vaccines have already been evaluated for their adverse events profiles and recommended by ACIP based on their safety records.
Table 2: Outcomes and Rankings
| Outcome | Importance* | Included in evidence profile |
|---|---|---|
| Incidence of hepatitis B | Important | Yes |
| Morbidity related to hepatitis B | Important | Yes |
| Mortality related to hepatitis B | Important | Yes |
| Serious adverse events associated with the 2-dose HepB vaccine* | Critical | Yes |
Table 3a. Summary of studies reporting seroprotection (SPR)*
| Study | Population | n/N (%) HBsAg-1018 (Heplisav-B) |
n/N (%) HBsAg-Eng (Engerix-B) |
Difference (95% CI) Risk ratio (95% CI) |
Study limitations (Risk of Bias) |
|---|---|---|---|---|---|
| Hyer, 2018 | HBV-10: 2,415 adults 18–55 years |
0/1,810 (0%) | 0/605 (0%) | — | Not serious |
| HBV-16: 2,449 adults 40–70 years |
3/1,968 (0.2%) | 2/481 (0.4%) | -0.3% (-0.8%, 0.3%) 0.37 (0.06, 2.19) |
Not serious | |
| HBV-23: 8,368 adults 18–70 years |
28/5,587 (0.5%) | 6/2,781 (0.2%) | 0.3% (0.03%, 0.5%) 2.32 (0.96, 5.60) |
Not serious | |
| Janssen, 2013 | 516 adults 18–75 years with chronic kidney disease |
10/254 (3.9%) | 8/262 (3.1%) | 0.9% (-2.3%, 4.1%) 1.29 (0.52, 3.21) |
Not serious |
| Bruxvoort, 2021 | 69,625 adults routinely vaccinated in a US health system | 52/31,183 (0.2%) | 71/38,442 (0.2%) | 0.0% (-0.1%, 0.0%) HR 0.92 (0.63, 1.39) |
Not serious |
Table 3b. Summary of Studies Reporting Serious Adverse Events
| Study | Population | n/N (%) HBsAg-1018 (Heplisav-B) |
n/N (%) HBsAg-Eng (Engerix-B) |
Difference (95% CI) Risk ratio (95% CI) |
Study limitations (Risk of Bias) |
|---|---|---|---|---|---|
| Halperin, 2006 | 99 healthy adults 18–28 years |
1/51 (2.0%) | 4/48 (8.3%) | -6.4% (-15.1%, 4.4%) 0.24 (0.03, 2.03) |
Not serious |
| Sablan, 2012 | 412 healthy adults 40–70 years |
10/206 (4.9%) | 13/206 (6.3%) | -1.5% (-5.9%, 3.0%) 0.77 (0.35, 1.71) |
Not serious |
| Janssen, 2013 | 516 adults 18–75 years with chronic kidney disease |
68/254 (26.8%) | 76/262 (29.0%) | -2.2% (-10.0%, 5.5%) 0.92 (0.70, 1.22) |
Not serious |
| Hyer, 2018 | HBV-10: 2,415 adults 18–55 years |
28/1,810 (1.5%) | 13/605 (2.1%) | -0.6% (-1.9%, 0.7%) 0.72 (0.38, 1.38) |
Not serious |
| HBV-16: 2,449 adults 40–70 years |
76/1,968 (3.9%) | 23/481 (4.8%) | -0.9% (-3.0%, 1.2%) 0.81 (0.51, 1.27) |
Not serious | |
| HBV-23: 8,368 adults 18–70 years |
345/5,587 (6.2%) | 148/2,781 (5.3%) | 0.9% (-0.2%, 1.9%) 1.16 (0.96, 1.40) |
Not serious |
Table 4. Grade Summary of Findings Table
| Certainty assessment | № of patients HBsAg-1018 | № of patients C HBsAg-Eng | Effect Relative (95% CI) | Effect Absolute (95% CI) | Certainty | Importance | ||||||
|---|---|---|---|---|---|---|---|---|---|---|---|---|
| № of studies | Study design | Risk of bias | Inconsistency | Indirectness | Imprecision | Other considerations | ||||||
| Cardiovascular events – RCTs | ||||||||||||
| 4 | randomized trials | not serious | serious a | not serious | serious b | none | 41/9619 (0.4%) | 16/4129 (0.4%) | RR 1.33 (0.58 to 3.08) |
128 more per 100,000 (from 163 fewer to 806 more) |
Type 3, Low | CRITICAL |
| Cardiovascular events – observational | ||||||||||||
| 1 | observational studies | not serious | not serious | not serious | serious b | none | 52/31183 (0.2%) | 71/38442 (0.2%) | HR 0.92 (0.63 to 1.32) |
15 fewer per 100,000 (from 68 fewer to 59 more) |
Type 4, Very Low | CRITICAL |
| Serious adverse events | ||||||||||||
| 6 | randomized trials | not serious | not serious | not serious | not serious | none | 528/9876 (5.3%) | 277/4383 (6.3%) | RR 0.96 (0.79 to 1.16) |
253 fewer per 100,000 (from 1,327 fewer to 1,011 more) |
Type 1, High | CRITICAL |
CI: Confidence interval; RR: Risk ratio; HR: Hazard Ratio
a. Heterogeneity of estimates across studies. I2 = 43%
b. Few events suggest fragility of the estimate. 95% CI cannot exclude the possibility of meaningful harm.
Appendix 1: Evidence retrieval strategies used for systematic review*
| Database | Strategy | Run Date |
|---|---|---|
| Medline
(OVID) 1946- |
hepatitis b vaccines/ OR ((hepatitis B ADJ5 vaccin*) OR (HBV ADJ5 vaccin*) OR recombivax hb OR engerix-b).ti,ab.
AND Exp Adults/ OR (adult* OR elder* OR senior*).ti,ab. AND Ae.fs OR ad.fs OR review.pt OR (dose* OR dosage* OR administration OR schedule* OR routine OR universal OR adverse OR efficacy OR effective* OR safe* OR strateg* OR risk* OR guideline* OR recommendation*).ti,ab. Limit to 2006 – ; Abstract Available |
12/4/2019, updated 9/20/2021 |
| Embase
(OVID) 1947- |
hepatitis b vaccine/ OR recombinant hepatitis B vaccine/ OR ((hepatitis B ADJ5 vaccin*) OR (HBV ADJ5 vaccin*) OR recombivax hb OR engerix-b).ti,ab.
AND Exp Adults/ OR (adult* OR elder* OR senior*).ti,ab. AND Ae.fs OR ad.fs OR do.fs. OR review.pt OR (dose* OR dosage* OR administration OR schedule* OR routine OR universal OR adverse OR efficacy OR effective* OR safe* OR strateg* OR risk* OR guideline* OR recommendation*).ti,ab. Limit to 2006 – ; NOT pubmed/medline; Abstract Available |
12/4/2019, updated 9/20/2021 |
| CINAHL
(Ebsco) |
(MH “Hepatitis B Vaccines+”) OR ((“hepatitis B” N5 vaccin*) OR (HBV N5 vaccin*) OR “recombivax hb” OR “engerix-b”)
AND (MH “Adult+”) OR (adult* OR elder* OR senior*) AND (dose* OR dosage* OR administration OR schedule* OR routine OR universal OR adverse OR efficacy OR effective* OR safe* OR strateg* OR risk* OR guideline* OR recommendation* OR review*) Limit to 2006 – ; exclude Medline records; Abstract Available |
12/4/2019, updated 9/20/2021 |
| Cochrane Library | [mh “Hepatitis B Vaccines”] OR ((“hepatitis B” N5 vaccin*) OR (HBV N5 vaccin*) OR “recombivax hb” OR “engerix-b”):ti,ab
AND (dose* OR dosage* OR administration OR schedule* OR routine OR universal OR adverse OR efficacy OR effective* OR safe* OR strateg* OR risk* OR guideline* OR recommendation* OR review*):ti,ab Limit to 2006- ; Abstract Available |
12/4/2019, updated 9/20/2021 |
*Exclusion criteria: articles dated earlier than year 2006, articles discussing vaccines not licensed in United States, articles not addressing the population of interest, and articles where data could not be abstracted