Hib vaccine
Vaccine description | |
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Target | Haemophilus influenzae type b |
Vaccine type | Conjugate |
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Trade names | ActHIB, Hiberix, OmniHIB, others |
AHFS/Drugs.com | Professional Drug Facts |
MedlinePlus | a607015 |
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Routes of administration | Intramuscular |
ATC code | |
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The Haemophilus influenzae type B vaccine, also known as Hib vaccine, is a vaccine used to prevent Haemophilus influenzae type b (Hib) infection.[2][3] In countries that include it as a routine vaccine, rates of severe Hib infections have decreased more than 90%.[2] It has therefore resulted in a decrease in the rate of meningitis, pneumonia, and epiglottitis.[4]
It is recommended by both the World Health Organization (WHO) and the U.S. Centers for Disease Control and Prevention (CDC).[2][5] Two or three doses should be given before six months of age.[2] In the United States a fourth dose is recommended between 12 and 15 months of age.[6] The first dose is recommended around six weeks of age with at least four weeks between doses.[2] If only two doses are used, another dose later in life is recommended.[2] It is given by injection into a muscle.[2]
Severe side effects are extremely rare.[2] About 20 to 25% of people develop pain at the site of injection while about 2% develop a fever.[2] There is no clear association with severe allergic reactions.[2] The Hib vaccine is available by itself, in combination with the diphtheria/tetanus/pertussis vaccine, and in combination with the hepatitis B vaccine, among others.[2] All Hib vaccines that are currently used are conjugate vaccine.[2]
An initial Hib vaccine consisting of plain (unconjugated) type b polysaccharide, was introduced in the United States in 1985.[7] but was replaced by a more effective conjugated formulations beginning in 1987.[8] As of 2013, 184 countries include it in their routine vaccinations.[2] It is on the World Health Organization's List of Essential Medicines.[9]
Medical uses
Hib conjugate vaccines have been shown to be effective against all manifestations of Hib disease, with a clinical efficacy among fully vaccinated children estimated to be between 95–100%. The vaccine has also been shown to be immunogenic in patients at high risk of invasive disease. Hib vaccine is not effective against non-type B Haemophilus influenzae. However, non-type B disease is rare in comparison to pre-vaccine rates of Haemophilus influenzae type B disease.[10]
Impact
Prior to introduction of the conjugate vaccine, Hib was a leading cause of childhood meningitis, pneumonia, and epiglottitis in the United States, causing an estimated 20,000 cases a year in the early 1980s. Nearly all disease was in children under five years old.[11] After routine use of Hib conjugate vaccines in the United States, the rate of invasive Hib disease decreased from 40–100 per 100,000 children down to fewer than 1 per 100,000.[12] Similar reductions in Hib disease occurred after introduction of the vaccine in Western Europe[13] and developing countries.[14] However, in recent years. Haemophilus influenzae strains with other encapsulated serotypes such as a or f, or non-encapsulated strains, have been recognized to cause invasive disease, particularly in high risk populations.[14]
Recommendations
The CDC and the WHO recommend that all infants be vaccinated using a polysaccharide-protein conjugate Hib vaccine, starting after the age of six weeks. The vaccination is also indicated in people without a spleen.[15]
Side effects
Clinical trials and ongoing surveillance have shown Hib vaccine to be safe. In general, adverse reactions to the vaccine are mild. The most common reactions are mild fever, loss of appetite, transient redness, swelling, or pain at the site of injection, occurring in 5–30% of vaccine recipients. More severe reactions are extremely rare.[citation needed]
Mechanisms of action
Polysaccharide vaccine
Haemophilus influenzae type b is a bacterium with a polysaccharide capsule; the main component of this capsule is polyribosyl ribitol phosphate (PRP). Anti-PRP antibodies have a protective effect against Hib infections. However, the antibody response to PRP was quite variable in young children, and diminished rapidly after administration. This problem was due to recognition of the PRP antigen by B cells, but not T cells. In other words, even though B cell recognition was taking place, T cell recruitment (via MHC class II) was not, which compromised the immune response. This interaction with only B cells is termed T-independent (TI). This process also inhibits the formation of memory B cells, thus compromising long term immune system memory.[16][17]
Conjugate vaccine
PRP covalently linked to a protein carrier was found to elicit a greater immune response than the polysaccharide form of the vaccine. This is due to the protein carrier being highly immunogenic in nature. The conjugate formulations show responses which are consistent with T-cell recruitment (namely a much stronger immune response). A memory effect (priming of the immune system against future attack by Hib) is also observed after administration; indicative that memory B cell formation is also improved over that of the unconjugated polysaccharide form. Since optimal contact between B cells and T cells is required (via MHC II) to maximize antibody production, it is reasoned that the conjugate vaccine allows B cells to properly recruit T cells, this is in contrast to the polysaccharide form in which it is speculated that B cells do not interact optimally with T cells leading to the TI interaction.[16][17]
Developing world
Introduction of Hib vaccine in developing countries lagged behind that in developed countries for several reasons. The expense of the vaccine was large in comparison to the standard EPI vaccines. Poor disease surveillance systems and inadequate hospital laboratories failed to detect the disease, leading many experts to believe that Hib did not exist in their countries. And health systems in many countries were struggling with the current vaccines they were trying to deliver.
GAVI and the Hib Initiative
In order to remedy these issues, the GAVI Alliance took active interest in the vaccine.[18][19][20]
History
Polysaccharide vaccine
The first Hib vaccine licensed was a unconjugated polysaccharide vaccine, called PRP. This vaccine was first marketed in the United States in 1985.[21] Similar to other unconjugated polysaccharide vaccines, serum antibody responses to PPP vaccine were highly age-dependent. Children under 18 months of age did not produce a positive response for this vaccine. As a result, the age group with the highest incidence of Hib disease was unprotected, limiting the usefulness of the vaccine. Also, post-licensure studies by Michael Osterholm[22] and his colleagues, and Dan M. Granoff et al.[23] suggested that the PRP vaccine was largely ineffective in preventing invasive Hib disease in children 18 to 59 months, the age group recommended for vaccination . The vaccine was withdrawn from the market in 1988.[24]
Conjugate vaccine
The shortcomings of the polysaccharide vaccine led to the production of the Hib polysaccharide-protein conjugate vaccine.[21] In 1987, the first Hib conjugate vaccine, which used diphtheria toxoid as the carrier protein (PRP-D), was licensed in the U.S. and initially recommended for children ages 18 to 59 months of age.[25] This vaccine was based on work done by Lasker Award-winning American scientists John Robbins and Rachel Schneerson[26] at the U.S. National Institutes of Health, and Porter Anderson and David Smith then at Boston Children's Hospital.[27] Attaching Hib polysaccharide to a protein carrier greatly increased the ability of the immune system of young children to recognize the polysaccharide and develop immunity. In contrast to unconjugated PRP vaccine, PRP-D vaccines was highly effective in controlling Hib disease in the age group being immunized (18 to 59 months). Unexpectedly. the vaccine also was associated with a dramatic decline in Hib disease in the age group less than 18 months, which at the time was not being vaccinated (evidence of indirect community protection or “herd immunity”.[28] Trudy Murphy and her colleagues reported that healthy children in a day care center who had been immunized with PRP-D had a lower rate of Hib colonization in their noses and throats than healthy unvaccinated children, which was not observed in children vaccinated with unconjugated PRP vaccine.[29] These results provided an explanation for the ability of PRP-D conjugate vaccine to lower transmission of Hib from conjugate-vaccinated to unvaccinated children, and provide indirect community protection from conjugate vaccination .
There are currently three types of conjugate vaccine, utilizing different carrier proteins for the conjugation process: inactivated tetanospasmin (also called tetanus toxoid); mutant diphtheria protein; and meningococcal group B outer membrane protein.[16] The Hib vaccine using a meningococcal outer membrane carrier protein has unique immunostimulatory properties, eliciting an anticapsular response to a single injection given to infants as young as 2 months of age.[30] In contrast, Hib conjugate vaccines using other protein carriers require two or three injections to reliably elicit anticapsular antibody responses in infants less than six months of age.[31]
Combination vaccines
Multiple combinations of Hib and other vaccines have been licensed in the United States, reducing the number of injections necessary to vaccinate a child. Hib vaccine combined with diphtheria-tetanus-pertussis–polio vaccines and hepatitis B vaccines are available in the United States. The World Health Organization (WHO) has certified several Hib vaccine combinations, including a pentavalent diphtheria-pertussis-tetanus-hepatitis B-Hib, for use in developing countries. There is not yet sufficient evidence on how effective this combined pentavalent vaccine is in relation to the individual vaccines.[32]
References
- ^ Professional Drug Facts
- ^ a b c d e f g h i j k l m World Health Organization (September 2013). "Haemophilus influenzae type b (Hib) Vaccination Position Paper – July 2013". Weekly Epidemiological Record. 88 (39): 413–426. hdl:10665/242126. PMID 24143842.
- ^ "WHO position on Haemophilus influenzae type b (Hib) vaccination-July 2013" (PDF). who.int. 27 October 2013. Archived (PDF) from the original on 19 January 2022. Retrieved 30 March 2016.
- ^ Mutsaerts EA, Madhi SA (2022). "11.3. Immunisation and vaccination". In Detels R, Karim QA, Baum F (eds.). Oxford Textbook of Global Public Health (7th ed.). Oxford University Press. pp. 584–589. ISBN 978-0-19-881680-5.
- ^ "Haemophilus b conjugate vaccines for prevention of Haemophilus influenzae type b disease among infants and children two months of age and older. Recommendations of the immunization practices advisory committee (ACIP)". MMWR. Recommendations and Reports. 40 (RR-1). cdc.gov: 1–7. January 1991. PMID 1899280.
- ^ "Hib (Haemophilus Influenzae Type B)". Archived from the original on 8 April 2016. Retrieved 30 March 2016.
- ^ Cochi SL, Fleming DW, Hull HF, Preblud SR, Orenstein WA (December 1986). "Haemophilus influenzae b polysaccharide vaccine. Physician acceptance and use of a new vaccine". American Journal of Diseases of Children. 140 (12): 1226–1230. doi:10.1001/archpedi.1986.02140260028019. PMID 3490784.
- ^ Weinberg GA, Granoff DM (October 1988). "Polysaccharide-protein conjugate vaccines for the prevention of Haemophilus influenzae type b disease". The Journal of Pediatrics. 113 (4): 621–631. doi:10.1016/S0022-3476(88)80369-X. PMID 3050001.
- ^ World Health Organization (2023). The selection and use of essential medicines 2023: web annex A: World Health Organization model list of essential medicines: 23rd list (2023). Geneva: World Health Organization. hdl:10665/371090. WHO/MHP/HPS/EML/2023.02.
- ^ Cox AD, Kuo Lee R, Ulanova M, Bruce MG, Tsang RS (January 2021). "Proceedings of a workshop to discuss the epidemiology of invasive Haemophilus influenzae disease with emphasis on serotype a and b in the Americas, 2019". Vaccine. 39 (4): 627–632. doi:10.1016/j.vaccine.2020.12.015. PMID 33358264. S2CID 229695991.
- ^ Broome CV (August 1987). "Epidemiology of Haemophilus influenzae type b infections in the United States". The Pediatric Infectious Disease Journal. 6 (8): 779–782. doi:10.1097/00006454-198708000-00036. PMID 3313240.
- ^ "Haemophilus influenzae Disease (Including Hib)". U.S. Centers for Disease Control and Prevention (CDC). 25 September 2012. Archived from the original on 30 January 2014. Retrieved 31 January 2014.
- ^ Whittaker R, Economopoulou A, Dias JG, Bancroft E, Ramliden M, Celentano LP (March 2017). "Epidemiology of Invasive Haemophilus influenzae Disease, Europe, 2007-2014". Emerging Infectious Diseases. 23 (3): 396–404. doi:10.3201/eid2303.161552. PMC 5382729. PMID 28220749.
- ^ a b Slack MP, Cripps AW, Grimwood K, Mackenzie GA, Ulanova M (June 2021). "Invasive Haemophilus influenzae Infections after 3 Decades of Hib Protein Conjugate Vaccine Use". Clinical Microbiology Reviews. 34 (3): e0002821. doi:10.1128/CMR.00028-21. PMC 8262803. PMID 34076491.
- ^ "Asplenia and Adult Vaccination". U.S. Centers for Disease Control and Prevention (CDC). 14 February 2019. Retrieved 29 March 2019.
- ^ a b c Kelly DF, Moxon ER, Pollard AJ (October 2004). "Haemophilus influenzae type b conjugate vaccines". Immunology. 113 (2): 163–174. doi:10.1111/j.1365-2567.2004.01971.x. PMC 1782565. PMID 15379976.
- ^ a b Finn A (1 January 2004). "Bacterial polysaccharide-protein conjugate vaccines". British Medical Bulletin. 70 (1): 1–14. doi:10.1093/bmb/ldh021. PMID 15339854.
- ^ "a new force in the fight against Hib meningitis and pneumonia". Hib Initiative (Press release). 8 December 2005. Retrieved 6 July 2024.
- ^ "Hib Initiative: a GAVI success story". Gavi, the Vaccine Alliance (Press release). 14 April 2010. Retrieved 6 July 2024.
- ^ "ADIPs and Hib Initiative Evaluation". Gavi, the Vaccine Alliance. 30 August 2019. Retrieved 6 July 2024.
- ^ a b Centers for Disease Control and Prevention (2006). Atkinson W, Hamborsky J, McIntyre L, Wolfe S (eds.). Epidemiology and Prevention of Vaccine-Preventable Diseases (9th ed.). Washington, D.C.: Public Health Foundation.
- ^ Osterholm MT, Rambeck JH, White KE, Jacobs JL, Pierson LM, Neaton JD, et al. (September 1988). "Lack of efficacy of Haemophilus b polysaccharide vaccine in Minnesota". JAMA. 260 (10): 1423–1428. doi:10.1001/jama.1988.03410100113035. PMID 3261350.
- ^ Granoff DM, Shackelford PG, Suarez BK, Nahm MH, Cates KL, Murphy TV, et al. (December 1986). "Hemophilus influenzae type B disease in children vaccinated with type B polysaccharide vaccine". The New England Journal of Medicine. 315 (25): 1584–1590. doi:10.1056/NEJM198612183152505. PMID 3491315.
- ^ Zarei AE, Almehdar HA, Redwan EM (20 January 2016). "Hib Vaccines: Past, Present, and Future Perspectives". Journal of Immunology Research. 2016: 7203587. doi:10.1155/2016/7203587. PMC 4745871. PMID 26904695.
- ^ "American Academy of Pediatrics Committee on Infectious Diseases: Haemophilus influenzae type b conjugate vaccine". Pediatrics. 81 (6): 908–911. June 1988. PMID 3259309.
- ^ "Haemophilus influenzae type b (Hib)". historyofvaccines.org. Retrieved 8 May 2023.
- ^ Robbins JB, Schneerson R, Anderson P, Smith DH (October 1996). "The 1996 Albert Lasker Medical Research Awards. Prevention of systemic infections, especially meningitis, caused by Haemophilus influenzae type b. Impact on public health and implications for other polysaccharide-based vaccines". JAMA. 276 (14): 1181–1185. doi:10.1001/jama.276.14.1181. PMID 8827975.
- ^ Murphy TV, White KE, Pastor P, Gabriel L, Medley F, Granoff DM, et al. (January 1993). "Declining incidence of Haemophilus influenzae type b disease since introduction of vaccination". JAMA. 269 (2): 246–248. doi:10.1001/jama.1993.03500020080036. PMID 8417244.
- ^ Murphy TV, Pastor P, Medley F, Osterholm MT, Granoff DM (April 1993). "Decreased Haemophilus colonization in children vaccinated with Haemophilus influenzae type b conjugate vaccine". The Journal of Pediatrics. 122 (4): 517–523. doi:10.1016/s0022-3476(05)83529-2. PMID 8463894.
- ^ Einhorn MS, Weinberg GA, Anderson EL, Granoff PD, Granoff DM (August 1986). "Immunogenicity in infants of Haemophilus influenzae type B polysaccharide in a conjugate vaccine with Neisseria meningitidis outer-membrane protein". Lancet. 2 (8502): 299–302. doi:10.1016/s0140-6736(86)90001-2. PMID 2874327.
- ^ Granoff DM, Anderson EL, Osterholm MT, Holmes SJ, McHugh JE, Belshe RB, et al. (August 1992). "Differences in the immunogenicity of three Haemophilus influenzae type b conjugate vaccines in infants". The Journal of Pediatrics. 121 (2): 187–194. doi:10.1016/s0022-3476(05)81186-2. PMID 1640282.
- ^ Bar-On ES, Goldberg E, Hellmann S, Leibovici L (April 2012). "Combined DTP-HBV-HIB vaccine versus separately administered DTP-HBV and HIB vaccines for primary prevention of diphtheria, tetanus, pertussis, hepatitis B and Haemophilus influenzae B (HIB)". The Cochrane Database of Systematic Reviews (4): CD005530. doi:10.1002/14651858.CD005530.pub3. PMC 11440342. PMID 22513932.
Further reading
- Ramsay M, ed. (2013). "Chapter 16: Haemophilus influenzae type b (Hib)". Immunisation against infectious disease. Public Health England.
- Hall E, Wodi AP, Hamborsky J, Morelli V, Schillie S, eds. (2021). "Chapter 8: Haemophilus influenzae". Epidemiology and Prevention of Vaccine-Preventable Diseases (14th ed.). Washington D.C.: U.S. Centers for Disease Control and Prevention (CDC).
External links
- "Haemophilus Influenzae Type b (Hib) Vaccine Information Statement". U.S. Centers for Disease Control and Prevention (CDC). 27 April 2023.
- "Haemophilus B Conjugate Vaccine (Meningococcal Protein Conjugate)". U.S. Food and Drug Administration (FDA). 7 November 2022.
- "Haemophilus b Conjugate Vaccine (Tetanus Toxoid Conjugate)". U.S. Food and Drug Administration (FDA). 14 October 2022.
- "Hiberix". U.S. Food and Drug Administration (FDA). 21 December 2023.