Hepatitis B Virus: A Comprehensive Strategy for Eliminating
Transmission in the United States Through Universal Childhood
Vaccination:
Recommendations of the Immunization Practices
Advisory Committee (ACIP)
CHAIRMAN
Samuel L. Katz, M.D. EXECUTIVE SECRETARY
Claire V. Broome, M.D. MEMBERS
* Stanley E. Broadnax, M.D.
American Academy of Pediatrics
Mary Lou Clements, M.D.
David W. Fraser, M.D.
* Caroline B. Hall, M.D.
Carlos E. Hernandez, M.D.
Gregory R. Istre, M.D.
Carlos H. Ramirez-Ronda, M.D.
Mary E. Wilson, M.D. |
EX OFFICIO MEMBERS
John La Montagne, Ph.D.
Carolyn Hardegree, M.D. LIAISON REPRESENTATIVES
American Academy of Family Physicians
Georges Peter, M.D.
Caroline B. Hall, M.D.
American College of Physicians
American Hospital Association
American Medical Association
Canadian National Advisory Committee on Immunization Department of Defense
Michael Peterson, D.V.M., M.P.H., Dr. P.H.
National Vaccine Program |
* Terms expired 6/30/91. |
The following statement updates all previous recommendations on protection against hepatitis B virus infection, including use of hepatitis B vaccine and hepatitis B immune globulin for prophylaxis against hepatitis B virus infection (MMWR 1985;34:313-24, 329-35, MMWR 1987;36:353-66, and MMWR 1990;39{No. RR-2}:8-19) and universal screening of pregnant women to prevent perinatal hepatitis B virus transmission (MMWR 1988;37:341-46, 51, and MMWR 1990;39{No. RR-2}:8-19). Recommendations concerning the prevention of other types of viral hepatitis are found in MMWR 1990;39(No. RR-2): 1-8, 22-26.
This document provides the rationale for a comprehensive strategy to eliminate transmission of hepatitis B virus in the United States. This prevention strategy includes making hepatitis B vaccine a part of routine vaccination schedules for all infants.
Immunization with hepatitis B vaccine is the most effective means of preventing HBV infection and its consequences. In the United States, most infections occur among adults and adolescents (2,3). The recommended strategy for preventing these infections has been the selective vaccination of persons with identified risk factors (1,2). However, this strategy has not lowered the incidence of hepatitis B, primarily because vaccinating persons engaged in high-risk behaviors, life-styles, or occupations before they become infected generally has not been feasible. In addition, many infected persons have no identifiable source for their infections and thus cannot be targeted for vaccination (2).
Preventing HBV transmission during early childhood is important because of the high likelihood of chronic HBV infection and chronic liver disease that occurs when children less than 5 years of age become infected (3). Testing to identify pregnant women who are hepatitis B surface antigen (HBsAg)-positive and providing their infants with immunoprophylaxis effec- tively prevents HBV transmission during the perinatal period (4,5). Integrating hepatitis B vaccine into childhood vaccination schedules in populations with high rates of childhood infection (e.g., Alaskan Natives and Pacific Islanders) has been shown to interrupt HBV transmission (6).
This document provides the rationale for a comprehensive strategy to eliminate transmission of HBV and ultimately reduce the incidence of hepatitis B and hepatitis B-associated chronic liver disease in the United States. The recommendations for implementing this strategy include making hepatitis B vaccine a part of routine vaccination schedules for infants.
Because screening selected pregnant women for HBsAg has failed to identify a high proportion of HBV-infected mothers (11,12), prenatal HBsAg testing of all pregnant women is now recommended (1,13,14). Universal prenatal testing would identify an estimated 22,000 HBsAg-positive women and could prevent at least 6,000 chronic HBV infections annually (3). Screening and vaccination programs for women and infants receiving care in the public sector have already been initiated through state immunization projects.
Horizontal transmission of HBV during the first 5 years of life occurs frequently in populations in which HBV infection is endemic. The risk of chronic infection is age dependent, ranging from 30% to 60% for children 1-5 years of age (15). Worldwide, it has been recommended that, in popula- tions in which HBV infection is acquired during childhood, hepatitis B vaccine should be integrated into routine vaccination schedules for infants, usually as a part of the World Health Organization's Expanded Programme on Immunization (16). In the United States, racial/ethnic groups shown to have high rates of childhood HBV infection include Alaskan Natives (6,17), Pacific Islanders (18), and infants of first-generation immigrant mothers from parts of the world where HBV infection is endemic, especially Asia (19,20). Vaccination programs to prevent perinatal, childhood, and adult HBV infections among Alaskan Natives were begun in late 1982; as a result, the incidence of acute hepatitis B in this population has declined by over 99% (6). Hepatitis B vaccine was integrated into vaccination schedules for infants in American Samoa beginning in 1986 and by 1990 was incorporated into the schedules of the remaining Pacific Islands under U.S. jurisdiction.
Each year, approximately 150,000 infants are born to women who have immigrated to the United States from areas of the world where HBV infection is highly endemic (3). Children born to HBsAg-positive mothers can be identified through prenatal screening programs. However, children born to HBsAg-negative immigrant mothers are still at high risk of acquiring HBV infection, usually from other HBV carriers in their families or communities (3,19,20). Infections among these children can be prevented by making hepatitis B vaccine part of their routine infant vaccinations (1).
The rates of HBV infection differ significantly among various racial and ethnic groups (2,21). For example, the prevalence of infection among adolescents and adults has been shown to be threefold to fourfold greater for blacks than for whites and to be associated with serologic evidence of previous infection with syphilis (21,22).
Efforts to vaccinate persons in the major risk groups have had limited success. For example, programs directed at injecting drug users failed to motivate them to receive three doses of vaccine (CDC, unpublished data). Health-care providers are often not aware of groups at high risk of HBV infection and frequently do not identify candidates for vaccination during routine health-care visits (CDC, unpublished data). In addition, there has been limited vaccination of susceptible household and sexual contacts of HBsAg carriers identified in screening programs for blood donors (23). Hepatitis B vaccination of health-care workers appears to have resulted in a substantial decrease in the rate of disease in this group, but has had little effect on overall rates of hepatitis B (2). Moreover, to achieve widespread vaccination of persons at occupational risk, regulations have had to be developed to ensure implementation of vaccination programs (24).
Educational programs to reduce parenteral drug use and unprotected sexual activity are important components of the strategy to prevent infection with the human immunodeficiency virus (HIV), which causes acquired immunodeficiency syndrome. These programs appear to have reduced the risk of HBV infections among homosexual men but have not had an impact on hepatitis B attributable to parenteral drug use or heterosexual trans- mission (2). Educational efforts alone are not likely to fully eliminate the high-risk behaviors responsible for HBV transmission.
Routes of transmission are similar to those of HBV. In the United States, HDV infection most commonly affects persons at high risk of HBV infection, particularly injecting drug users and persons receiving clotting factor concentrates (26). Preventing acute and chronic HBV infection of susceptible persons will also prevent HDV infection.
Infants and children can receive hepatitis B vaccine during routine health-care visits; no additional visits would be required. Costs include that of the vaccine and the incremental expense associated with delivering an additional vaccine during a scheduled health-care visit. Implementation of this immunization strategy would be greatly facilitated by the develop- ment and use of multiple-antigen vaccines (e.g., diphtheria-tetanus- pertussis {DTP}/hepatitis B, Haemophilus influenzae type b conjugate/ hepatitis B). These vaccines would reduce the number of injections received by the infant, reduce the cost of administration, and greatly facilitate widespread vaccine delivery.
Since most HBV infections occur among adults, disease control could be accelerated by vaccinating emerging at-risk populations, such as adoles- cents and susceptible contacts of chronic HBV carriers. The recommendation for universal infant vaccination neither precludes vaccinating adults identified to be at high risk of infection nor alters previous recommen- dations for postexposure prophylaxis for hepatitis B (1).
The reduction in acute hepatitis B and hepatitis B-associated chronic liver disease resulting from universal infant vaccination may not become apparent for a number of years. However, universal HBsAg screening of pregnant women to prevent perinatal HBV infection has been shown to be cost saving (28, CDC, unpublished data), and the estimated cost of universal hepatitis B vaccination for infants is less than the direct medical and work-loss costs associated with the estimated 5% lifetime risk of infection (CDC, unpublished data). Currently, the cost of an infant's dose of hepatitis B vaccine delivered in the public sector is about the same as each of the other childhood vaccinations. Vaccinating adolescents and adults is substantially more expensive because of the higher vaccine cost and the higher implementation costs of delivering vaccine to target populations. In the long term, universal infant vaccination would eliminate the need for vaccinating adolescents and high-risk adults.
The recombinant vaccines are produced by using HBsAg synthesized by Saccharomyces cerevisiae (common bakers' yeast), into which a plasmid containing the gene for HBsAg has been inserted. Purified HBsAg is obtained by lysing the yeast cells and separating HBsAg from the yeast components by biochemical and biophysical techniques. Hepatitis B vaccines are packaged to contain 10-40 ug of HBsAg protein/mL after adsorption to aluminum hydroxide (0.5 mg/mL); thimerosal (1:20,000 concentration) is added as a preservative.
Routes and sites of administration.
The recommended series of three intramuscular doses of hepatitis B vaccine induces a protective antibody response (anti-HBs >=10 milli-inter- national units {mIU}/mL) in >90% of healthy adults and in >95% of infants, children, and adolescents (31-33). Hepatitis B vaccine should be admin- istered only in the deltoid muscle of adults and children or in the antero- lateral thigh muscle of neonates and infants; the immunogenicity of the vaccine for adults is substantially lower when injections are administered in the buttock (34). When hepatitis B vaccine is administered to infants at the same time as other vaccines, separate sites in the anterolateral thigh may be used for the multiple injections. This method is preferable to administering vaccine at sites such as the buttock or deltoid.
Compared with three standard doses admistered intramuscularly, three low doses of plasma-derived or recombinant vaccine administered intra- dermally to adults result in lower seroconversion rates (55%-81%) and lower final titers of anti-HBs (35-38), although four doses of plasma-derived vaccine administered intradermally have produced responses comparable with vaccine administered intramuscularly (39). Plasma-derived vaccine admin- istered intradermally to infants and children does not induce an adequate antibody response (40). At this time, low-dose intradermal vaccination of adults should be performed only under research protocol with written informed consent. Persons who have been vaccinated intradermally should be tested for anti-HBs. Those with an inadequate response (anti-HBs <10 mIU/ mL) should be revaccinated with three full doses of vaccine administered intramuscularly. Intradermal vaccination should not be used for infants or children.
Vaccination during pregnancy.
On the basis of limited experience, there is no apparent risk of adverse effects to developing fetuses when hepatitis B vaccine is admin- istered to pregnant women (CDC, unpublished data). The vaccine contains noninfectious HBsAg particles and should cause no risk to the fetus. HBV infection affecting a pregnant woman may result in severe disease for the mother and chronic infection for the newborn. Therefore, neither pregnancy nor lactation should be considered a contraindication to vaccination of women.
Each vaccine has been evaluated to determine the age-specific dose at which an optimum antibody response is achieved. The recommended dose varies by product and the recipient's age and, for infants, by the mother's HBsAg serologic status (Table 1). In general, the vaccine dose for children and adolescents is 50%-75% lower than that required for adults (Table 1).
Incorporating hepatitis B vaccine into childhood vaccination schedules may require modifications of previously recommended schedules. However, a protective level of anti-HBs (>=10 mIU/mL) was achieved when hepatitis B vaccine was administered in a variety of schedules, including those in which vaccination was begun soon after birth (5,8,41).
In a three-dose schedule, increasing the interval between the first and second doses of hepatitis B vaccine has little effect on immunogenicity or final antibody titer. The third dose confers optimal protection, acting as a booster dose. Longer intervals between the last two doses (4-12 months) result in higher final titers of anti-HBs (42,43). Several studies have shown that the currently licensed vaccines produce high rates of serocon- version (>95%) and induce adequate levels of anti-HBs when administered to infants at birth, 2 months, and 6 months of age or at 2 months, 4 months, and 6 months of age (CDC, Merck Sharpe & Dohme, SmithKline Beecham, unpub- lished data). When the vaccine is administered in four doses at 0, 1, 2, and 12 months, the last dose is necessary to ensure the highest final antibody titer.
When hepatitis B vaccine has been administered at the same time as other vaccines, no interference with the antibody response of the other vaccines has been demonstrated (44).
If the vaccination series is interrupted after the first dose, the second dose should be administered as soon as possible. The second and third doses should be separated by an interval of at least 2 months. If only the third dose is delayed, it should be administered when convenient.
The immune response when one or two doses of a vaccine produced by one manufacturer are followed by subsequent doses from a different manufacturer has been shown to be comparable with that resulting from a full course of vaccination with a single vaccine.
Larger vaccine doses or an increased number of doses are required to induce protective antibody in a high proportion of hemodialysis patients (45,46) and may also be necessary for other immunocompromised persons (e.g., those who take immunosuppressive drugs or who are HIV positive), although few data are available concerning response to higher doses of vaccine by these patients (47).
Prevaccination testing for susceptibility. Susceptibility testing is not indicated for immunization programs for children or for most adoles- cents because of the low rate of HBV infection and the relatively low cost of vaccine. For adults, the decision to do prevaccination testing should include an analysis of cost effectiveness because of the higher cost of the vaccine. Testing for prior infection should be considered for adults in risk groups with high rates of HBV infection (e.g., injecting drug users, homosexual men, and household contacts of HBV carriers). The decision for testing should be based on whether the costs of testing balance the costs of vaccine saved by not vaccinating already-infected persons. Estimates of the cost effectiveness of testing depend on three variables: the cost of vaccination, the cost of testing for susceptibility, and the expected prevalence of immune persons. If susceptibility testing is being considered, careful attention should also be given to the likelihood of patient follow-up and vaccine delivery.
For routine testing, only one antibody test is necessary (antibody either to the core antigen {anti-HBc} or anti-HBs). Anti-HBc testing identifies all previously infected persons, including HBV carriers, but does not differentiate carriers and non-carriers. The presence of anti-HBs identifies previously infected persons, except for HBV carriers. Neither test has a particular advantage for groups expected to have HBV carrier rates <2%, such as health-care workers. Anti-HBc may be preferable so that unnecessary vaccination of HBV carriers can be avoided in groups with high carrier rates.
Postvaccination testing for serologic response. Such testing is not necessary after routine vaccination of infants, children, or adolescents. Testing for immunity is advised only for persons whose subsequent clinical management depends on knowledge of their immune status (e.g., infants born to HBsAg-positive mothers, dialysis patients and staff, and persons with HIV infection). Postvaccination testing should also be considered for persons at occupational risk who may have exposures from injuries with sharp instruments, because knowledge of their antibody response will aid in determining appropriate postexposure prophylaxis. When necessary, postvac- cination testing should be performed from 1 to 6 months after completion of the vaccine series. Testing after immunoprophylaxis of infants born to HBsAg-positive mothers should be performed from 3 to 9 months after the completion of the vaccination series (see section on Postexposure prophylaxis).
Revaccination of nonresponders. When persons who do not respond to the primary vaccine series are revaccinated, 15%-25% produce an adequate antibody response after one additional dose and 30%-50% after three additional doses (48). Therefore, revaccination with one or more additional doses should be considered for persons who do not respond to vaccination initially.
After a person has been exposed to HBV, appropriate immunoprophylactic treatment can effectively prevent infection. The mainstay of postexposure immunoprophylaxis is hepatitis B vaccine, but in some settings the addition of HBIG will provide some increase in protection. Table 2 provides a guide to recommended treatment for various HBV exposures.
Transmission of perinatal HBV infection can be effectively prevented if the HBsAg-positive mother is identified and if her infant receives appro- priate immunoprophylaxis. Hepatitis B vaccination and one dose of HBIG, administered within 24 hours after birth, are 85%-95% effective in preventing both HBV infection and the chronic carrier state (4,5,8). Hepatitis B vaccine administered alone in either a three-dose or four-dose schedule (Table 1), beginning within 24 hours after birth, is 70%-95% effective in preventing perinatal HBV infections (8,41). The infants of women admitted for delivery who have not had prenatal HBsAg testing pose problems in clinical management. Initiating hepatitis B vaccination at birth for infants born to these women will provide adequate postexposure prophylaxis if the mothers are indeed HBsAg positive. The few infections not prevented by either of these treatment regimens were most likely acquired in utero or may be due to very high levels of maternal HBV-DNA (49).
Serologic testing of infants who receive immunoprophylaxis to prevent perinatal infection should be considered as an aid in the long-term medical management of the few infants who become HBV carriers. Testing for anti-HBs and HBsAg at 9-15 months of age will determine the success of the therapy and, in the case of failure, will identify HBV carriers or infants who may require revaccination.
Recommendations for postexposure prophylaxis in circumstances other than the perinatal period (Table 2) have been addressed in a previous statement and are reprinted as Appendix A to this document.
The duration of vaccine-induced immunity has been evaluated in long- term follow-up studies of both adults and children (48,51). Only the plasma-derived hepatitis B vaccine has been evaluated because it has had the longest clinical use; however, on the basis of comparable immunogen- icity and short-term efficacy, similar results would be expected with recombinant vaccines. The magnitude of the antibody response induced by the primary vaccination series is predictive of antibody persistence, and a logarithmic decline of antibody levels occurs over time. Among young adults (homosexual men and Alaskan Eskimos) who initially responded to a three- dose vaccine series, loss of detectable antibody has ranged from 13% to 60% after 9 years of follow-up. For children vaccinated after the first year of life, the rate of antibody decline has been lower than for adults (51). The peak antibody titers for infants are lower than those for children immunized after 12 months of age, but the rate of antibody decline is comparable with that observed for adults in the same population.
Long-term studies of healthy adults and children indicate that immuno- logic memory remains intact for at least 9 years and confers protection against chronic HBV infection, even though anti-HBs levels may become low or decline below detectable levels (48,51,52). In these studies, the HBV infections were detected by the presence of anti-HBc. No episodes of clinical hepatitis were reported and HBsAg was not detected, although brief episodes of viremia may not have been detected because of infrequent testing. The mild, inapparent infections among persons who have been previously vaccinated should not produce the sequelae associated with chronic HBV infection and should provide lasting immunity. In general, follow-up studies of children vaccinated at birth to prevent perinatal HBV infection have shown that a continued high level of protection from chronic HBV infections persists at least 5 years (52,53).
For children and adults whose immune status is normal, booster doses of vaccine are not recommended, nor is serologic testing to assess antibody levels necessary. The possible need for booster doses will be assessed as additional information becomes available. For hemodialysis patients, vaccine-induced protection may be less complete and may persist only as long as antibody levels are >=10 mIU/mL. For these patients, the need for booster doses should be assessed by annual antibody testing, and a booster dose should be administered when antibody levels decline to <10 mIU/mL.
Vaccine-associated side effects
Pain at the injection site (3%-29%) and a temperature greater than 37.7 C (1%-6%) have been among the most frequently reported side effects among adults and children receiving vaccine (5,31-33,50). In placebo-controlled studies, these side effects were reported no more frequently among vaccinees than among persons receiving a placebo (33,50). Among children receiving both hepatitis B vaccine and DTP vaccine, these mild side effects have been observed no more frequently than among children receiving DTP vaccine alone.
Serious adverse events
In the United States, surveillance of adverse reactions has shown a possible association between Guillain-Barre syndrome (GBS) and receipt of the first dose of plasma-derived hepatitis B vaccine (54, CDC unpublished data). GBS was reported at a very low rate (0.5/100,000 vaccinees), no deaths were reported, and all reported cases were among adults. An estimated 2.5 million adults received one or more doses of recombinant hepatitis B vaccine during the period 1986-1990. Available data from reporting systems for adverse events do not indicate an association between receipt of recombinant vaccine and GBS (CDC, unpublished data).
Until recently, large-scale hepatitis B vaccination programs for infants (e.g., Taiwan, Alaska, and New Zealand) have primarily used plasma- derived hepatitis B vaccine. No association has been found between vaccin- ation and the occurrence of severe adverse events, including seizures and GBS (55, B. McMahon and A. Milne, unpublished data). However, systematic surveillance for adverse reactions has been limited in these populations, and only a small number of children have received recombinant vaccine. Any presumed risk of adverse events possibly associated with hepatitis B vaccination must be balanced against the expected risk of acute and chronic liver disease associated with the current 5% lifetime risk of HBV infection in the United States. It is estimated that, for each U.S. birth cohort, 2,000-5,000 persons will die from HBV-related liver disease.
As hepatitis B vaccine is introduced for routine vaccination of infants, surveillance for vaccine-associated adverse events will continue to be an important part of the program in spite of the current record of safety. Any adverse event suspected to be associated with hepatitis B vaccination should be reported to the Vaccine Adverse Event Reporting System (VAERS). VAERS forms can be obtained by calling 1-800-822-7967.
Universal Vaccination of Infants Born to HBsAg-Negative Mothers
The 0-, 1-, and 6-month schedule is preferred for vaccinating adoles- cents with the age-appropriate dose of vaccine (Table 1). However, the choice of vaccination schedule should take into account the feasibility of delivering three doses of vaccine over a given period of time. The use of alternate schedules (e.g., 0, 2, and 4 months) may be advisable to achieve complete vaccination.
For persons in health-care fields, vaccination should be completed during training in schools of medicine, dentistry, nursing, laboratory technology, and other allied health professions, before trainees have their first contact with blood.
Staff of nonresidential day-care programs for the develop- mentally disabled (e.g., schools, sheltered workshops) attended by known HBV carriers have a risk of infection comparable with that of health-care workers and therefore should be vaccinated (60). The risk of infection for other clients appears to be lower than the risk for staff. Vaccination of clients in day care programs may be considered. Vaccination of classroom contacts is strongly encouraged if a classmate who is an HBV carrier behaves aggres- sively or has special medical problems (e.g., exudative dermatitis, open skin lesions) that increase the risk of exposure to his or her blood or serous secretions.
TABLE 1. Recommended doses of currently licensed hepatitis B vaccines ================================================================================================ Recombivax HB * Engerix-B * ------------------ ------------------ Group Dose (ug) (mL) Dose (ug) (mL) -------------------------------------------------------------------------- Infants of HBsAg† -negative mothers and children <11 years 2.5 (0.25) 10 (0.5) Infants of HBsAg-positive mothers; prevention of 5 (0.5) 10 (0.5) perinatal infection Children and adolescents 11-19 years 5 (0.5) 20 (1.0) Adults >=20 years 10 (1.0) 20 (1.0) Dialysis patients and other immunocompromised persons 40 (1.0) § 40 (2.0) ¶ -------------------------------------------------------------------------- * Both vaccines are routinely administered in a three-dose series. Engerix-B has also been licensed for a four-dose series administered at 0, 1, 2, and 12 months. † HBsAg = Hepatitis B surface antigen. § Special formulation. ¶ Two 1.0-mL doses administered at one site, in a four-dose schedule at 0, 1, 2, and 6 months. ================================================================================================
TABLE 2. Guide to postexposure immunoprophylaxis for exposure to hepatitis B virus ==================================================================================== Type of exposure Immunoprophylaxis ------------------------------------------------------------------------------- Perinatal Vaccination + HBIG * Sexual -- acute infection HBIG +/- Vaccination Sexual -- chronic carrier Vaccination Household contact -- chronic carrier Vaccination Household contact -- None unless acute case known exposure Household contact -- acute case, known exposure HBIG +/- vaccination Infant (<12 months) -- acute case in primary HBIG + vaccination care-giver Inadvertent -- percutaneous/ permucosal Vaccination +/- HBIG ------------------------------------------------------------------------------- * HBIG = Hepatitis B immune globulin. ====================================================================================
TABLE 3. Recommended schedule of hepatitis B immunoprophylaxis to prevent perinatal transmission of hepatitis B virus infection ====================================================================================================== -------------------------------------------------------------------------------------- Infant born to mother known to be HBsAg * positive Vaccine dose Age of infant First Birth (within 12 hours) HBIG § Birth (within 12 hours) Second 1 month Third 6 months ¶ Infant born to mother not screened for HBsAg Vaccine dose ** Age of infant First Birth (within 12 hours) HBIG § If mother is found to be HBsAg positive, administer dose to infant as soon as possible, not later than 1 week after birth Second 1-2 months Third 6 months ¶ -------------------------------------------------------------------------------------- * HBsAg = Hepatitis B surface antigen. See Table 1 for appropriate vaccine dose. § Hepatitis B immune globulin (HBIG) -- 0.5 mL administered intramuscularly at a site different from that used for vaccine. ¶ If four-dose schedule (Engerix-B) is used, the third dose is administered at 2 months of age and the fourth dose at 12-18 months. ** First dose = dose for infant of HBsAg-positive mother (see Table 1). If mother is found to be HBsAg positive, continue that dose; if mother is found to be HBsAg negative, use appropriate dose from Table 1. Infants of women who are HBsAg negative can be vaccinated at 2 months of age. ======================================================================================================
TABLE 4. Recommended schedules of hepatitis B vaccination for infants born to HBsAg * -negative mothers ============================================================================================== Hepatitis B vaccine Age of infant ---------------------------------------------------------------------------------- Option 1 Dose 1 Birth -- before hospital discharge Dose 2 1-2 months Dose 3 6-18 months Option 2 Dose 1 1-2 months Dose 2 4 months Dose 3 6-18 months ---------------------------------------------------------------------------------- * HBsAg = Hepatitis B surface antigen. Hepatitis B vaccine can be administered simultaneously with diphtheria-tetanus-pertussis, Haemophilus influenzae type b conjugate, measles-mumps-rubella, and oral polio vaccines at the same visit. ==============================================================================================
APPENDIX A: Postexposure Prophylaxis for Hepatitis B
SOURCE: MMWR 40(RR-13);21-25 DATE: Nov 22, 1991
Adapted from: CDC. Protection against viral hepatitis: recommendations of the Immunization Practices Advisory Committee (ACIP). MMWR 1990;39(No. RR-2):17-22.
Various studies have established the relative efficacies of HBIG and/or hepatitis B vaccine in different exposure situations. For an infant with perinatal exposure to an HBsAg-positive and HBeAg-positive mother, a regimen combining one dose of HBIG at birth with the hepatitis B vaccine series started soon after birth is 85%-95% effective in preventing develop- ment of the HBV carrier state (A1-A3). Regimens involving either multiple doses of HBIG alone or the vaccine series alone have 70%-90% efficacy (A4,A5).
For inadvertent perrcutaneous exposure, only regimens including HBIG and/or immune globulin (IG) have been studied. A regimen of two doses of HBIG, one given after exposure and one a month later, is about 75% effective in preventing hepatitis B in this setting (A6,A7). For sexual exposure to a person with acute hepatitis B, a single dose of HBIG is 75% effective if administered within 2 weeks of last sexual exposure (A8). The efficacy of IG for postexposure prophylaxis is uncertain; IG no longer has a role in postexposure prophylaxis of hepatitis B because of the avail- ability of HBIG and the wider use of hepatitis B vaccine.
Recommendations on postexposure prophylaxis are based on available efficacy data and on the likelihood of future HBV exposure for the person requiring treatment. In all exposures, a regimen combining HBIG with hepatitis B vaccine will provide both short- and long-term protection, will be less costly than the two-dose HBIG treatment alone, and is the treatment of choice.
After any such exposure, a blood sample should be obtained from the person who was the source of the exposure and should be tested for HBsAg. The hepatitis B vaccination status and anti-HBs response status (if known) of the exposed person should be reviewed. The outline below and Table A1 summarize prophylaxis for percutaneous or permucosal exposure to blood according to the HBsAg status of the source of exposure and the vaccination status and vaccine response of the exposed person. For greatest effectiveness, passive prophylaxis with HBIG, when indicated, should be administered as soon as possible after exposure since its value beyond 7 days after exposure is unclear.
Treatment when source is found to be | |||
---|---|---|---|
Exposed person | HBsAg positive | HBsAg negative | Unknown or not tested |
Unvaccinated | Administer HBIG x 1* and initiate hepatitis B vaccine |
Initiate hepatitis B vaccine |
Initiate hepatitis B vaccine |
Previously vaccinated Known responder |
Test exposed person for anti-HBs
|
No treatment | No treatment |
Known non-responder | HBIG x 2 or HBIG x 1, plus 1 dose of hepatitis B vaccine |
No treatment | If known high-risk source, may treat as if source were HBsAg positive |
Response unknown | Test exposed person for anti-HB§
|
No treatment | Test exposed person for anti-HBs§
|
*Hepatitis B immune globulin (HBIG) dose 0.06 mL/Kg intramuscularly.
Hepatitis B vaccine dose-see Table 1. §Adequate anti-HBs is >=10 milli-international units. |
All susceptible persons whose sex partners have acute hepatitis B infection should receive a single dose of HBIG (0.06 mL/kg) and should begin the hepatitis B vaccine series if prophylaxis can be started within 14 days of the last sexual contact or if sexual contact with the infected person will continue. Administering the vaccine with HBIG may improve the efficacy of postexposure treatment. The vaccine has the added advantage of conferring long-lasting protection.
An alternate treatment for persons who are not from a high-risk group for whom vaccine is routinely recommended and whose regular sex partners have acute HBV infection is to administer one dose of HBIG (without vaccine) and retest the sex partner for HBsAg 3 months later. No further treatment is necessary if the sex partner becomes HBsAg negative. If the sex partner remains HBsAg positive, a second dose of HBIG should be given and the hepatitis B vaccine series started.
References
A1. Stevens CE, Taylor PE, Tong MJ, et al. Yeast-recombinant hepatitis B vaccine: efficacy with hepatitis B immune globulin in prevention of perinatal hepatitis B virus transmission. JAMA 1987;257:2612-6.
A2. Beasley RP, Hwang L-Y, Lee G-C, et al. Prevention of perinatally trans- mitted hepatitis B virus infections with hepatitis B immune globulin and hepatitis B vaccine. Lancet 1983;2:1099-102.
A3. Stevens CE, Toy P, Tong MJ, et al. Perinatal hepatitis B virus trans- mission in the United States: prevention by passive-active immuni- zation. JAMA 1985;253:1740-5.
A4. Beasley RP, Hwang L-Y, Stevens CE, et al. Efficacy of hepatitis B immune globulin for prevention of perinatal transmission of the hepatitis B virus carrier state: final report of a randomized double- blind, placebo-controlled trial. Hepatology 1983;3:135-41.
A5. Xu Z-Y, Liu C-B, Francis DP, et al. Prevention of perinatal acquisition of hepatitis B virus carriage using vaccine: preliminary report of a randomized, double-blind placebo-controlled and comparative trial. Pediatrics 1985;76:713-8.
A6. Seeff LB, Wright EC, Zimmerman HJ, et al. Type B hepatitis after needlestick exposure. Prevention with hepatitis B immune globulin: final report of the Veterans Administration Cooperative Study. Ann Intern Med 1978;88:285-93.
A7. Grady GF, Lee VA, Prince AM, et al. Hepatitis B immune globulin for accidental exposures among medical personnel: final report of a multi- center controlled trial. J Infect Dis 1978; 138:625-38.
A8. Redeker AG, Mosley JW, Gocke DJ, McKee AP, Pollack W. Hepatitis B immune globulin as a prophylactic measure for spouses exposed to acute type B hepatitis. N Engl J Med 1975;293:1055-9.
* An adequate antibody level is >=10 mIU/mL.
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