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Hepatitis A vaccine

From Wikipedia, the free encyclopedia
Vaccine to prevent hepatitis A

Pharmaceutical compound
Hepatitis A vaccine
Havrix junior monodose (hepatitis A) for children
Vaccine description
TargetHepatitis A virus
Vaccine typeInactivated or attenuated
Clinical data
Trade namesHavrix, others
AHFS/Drugs.comMonograph
MedlinePlusa695003
Pregnancy
category
Routes of
administration		Intramuscular
ATC code
Legal status
Legal status
Identifiers
DrugBank
ChemSpider
  • none
UNII
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Hepatitis A vaccine is avaccine that preventshepatitis A.[2][3] It is effective in around 95% of cases and lasts for at least twenty years and possibly a person's entire life.[4] If given, two doses are recommended beginning after the age of one.[2] It is given byinjection into a muscle.[2] The first hepatitis A vaccine was approved in the European Union in 1991, and the United States in 1995.[5] It is on theWorld Health Organization's List of Essential Medicines.[6]

TheWorld Health Organization (WHO) recommends universal vaccination in areas where the disease is moderately common.[2] Where the disease is very common, widespread vaccination is not recommended as people typically develop immunity through infection during childhood.[2] The USCenters for Disease Control and Prevention (CDC) recommends vaccinating:[7]

In addition, a person who has not previously received hepatitis A vaccine and who has direct contact with someone with hepatitis A should get hepatitis A vaccine within two weeks after exposure.[8]

Severe side effects are very rare.[2] Pain at the site of injection occurs in about 15% of children and half of adults.[2] Most hepatitis A vaccines contain inactivated virus while a few contain weakened virus.[2] The ones with weakened virus are not recommended duringpregnancy or in those withpoor immune function.[2] A few formulations combine hepatitis A with eitherhepatitis B ortyphoid vaccine.[2]

Soreness or redness where the shot is given, fever, headache, tiredness, or loss of appetite can happen after receiving the hepatitis A vaccine. As with any medicine, there is a very remote chance of a vaccine causing a severe allergic reaction, other serious injury, or death.[8]


Medical uses

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Within the US, the vaccine Vaqta, developed byMaurice Hilleman and his team atMerck & Co. was licensed in 1995.[9][10][11] The vaccine was phased in, around 1996, for children living in high-risk areas. In 1999, its usage was widened to areas with elevated levels of infection. In the US as of 2007[update], the vaccine is strongly recommended for all children 12 to 23 months of age in an attempt to eradicate the virus nationwide. Although the originalFood and Drug Administration (FDA) license for Havrix byGlaxoSmithKline is dated 1995,[12] it had been approved in Europe in 1991.[5]

The USCenters for Disease Control and Prevention (CDC) recommends vaccination of all children over one year of age, people whose sexual activity puts them at risk, people with chronic liver disease, people who are being treated with clotting factor concentrates, people working near the virus, and people who are living in communities where an outbreak is present.[13] Hepatitis A is the most common vaccine-preventable virus acquired during travel,[14] so people traveling to places where the virus is common like the Indian subcontinent, Africa, Central America, South America, Asia, and Eastern Europe should be vaccinated.[13][15]

The vaccine is given in the muscle of the upper arm, in two doses for the best protection. The initial dose of the vaccine should be followed up by a booster six to twelve months later.[13] Protection against hepatitis A begins approximately two to four weeks after the initial vaccination.[13][15] Protection lasts at least 15 years and is estimated to last at least 25 years if the booster is administered.[16]

ACochrane review found that both types of vaccines offer significant protection, for at least two years using the inactivated vaccine and at least five years with the attenuated vaccine. The review concluded that the inactivated vaccine is safe, but required more high-quality evidence to assess the safety of the attenuated vaccine.[17][needs update]

Commercial vaccines

[edit]
Havrix vaccine

Several commercial hepatitis A vaccines are available. The definition of (U)nits varies among manufacturers depending on how hepatitis A antigen is measured in their products.

  • Avaxim: made bySanofi Pasteur. Inactivated hepatitis A virus produced inMRC-5 cells. Each dose contains 160 U of antigen adsorbed onaluminium hydroxide (0.3 mg Al).[18]
  • Epaxal: made byCrucell. Also sold under the brand names HAVpur and VIROHEP-A. This vaccine consists ofvirosomes, artificial particles composed of syntheticlipids andinfluenza proteins in addition to the hepatitis A antigen. It does not containaluminium.[19]
  • Havrix: made byGlaxoSmithKline. Inactivated hepatitis A virus produced in MRC-5 cells. Each adult dose contains 1440ELISA units of viral antigen adsorbed on aluminium hydroxide (0.5 mg Al). The pediatric (child) doses contain half the amount of viral antigen and aluminium.[20]
  • Vaqta: made byMerck. Inactivated hepatitis A virus produced in MRC-5 cells. An adult dose contains 50 U of antigen adsorbed onto 0.45 mg of aluminium (as aluminium hydroxyphosphate sulfate); a child dose contains half the amounts of antigen and aluminium.[21]

Combination vaccines

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References

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  1. ^"Havrix - referral".European Medicines Agency. 27 June 2024. Retrieved12 July 2024.
  2. ^abcdefghijWorld Health Organization (2012). "WHO position paper on hepatitis A vaccines – June 2012".Weekly Epidemiological Record.87 (28/29):261–76.hdl:10665/241938.PMID 22905367.
  3. ^World Health Organization (2022). "WHO position paper on hepatitis A vaccines – October 2022".Weekly Epidemiological Record.97 (40):493–512.hdl:10665/363397.
  4. ^"Clinical Overview of Hepatitis A". 19 January 2022.
  5. ^abPatravale V, Dandekar P, Jain R (2012).Nanoparticulate drug delivery perspectives on the transition from laboratory to market (1. publ. ed.). Oxford: Woodhead Pub. p. 212.ISBN 978-1-908818-19-5.
  6. ^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.
  7. ^Nelson NP, Weng MK, Hofmeister MG, Moore KL, Doshani M, Kamili S, et al. (July 2020)."Prevention of Hepatitis A Virus Infection in the United States: Recommendations of the Advisory Committee on Immunization Practices, 2020"(PDF).MMWR. Recommendations and Reports.69 (5):1–38.doi:10.15585/mmwr.rr6905a1.PMC 8631741.PMID 32614811.
  8. ^abc"Hepatitis A Vaccine Information Statement". U.S.Centers for Disease Control and Prevention (CDC). October 2021. Retrieved13 July 2022.Public Domain This article incorporates text from this source, which is in thepublic domain.
  9. ^"Hepatitis A: Vaccine Licensed | History of Vaccines".historyofvaccines.org. Archived fromthe original on 21 January 2022. Retrieved6 February 2021.
  10. ^Tulchinsky TH (2018). "Maurice Hilleman: Creator of Vaccines That Changed the World".Case Studies in Public Health. pp. 443–470.doi:10.1016/B978-0-12-804571-8.00003-2.ISBN 978-0-12-804571-8.
  11. ^"Materials Documenting the Contribution of Dr. Maurice Hilleman to the Millennium Time Capsule Ceremony".National Museum of American History. Retrieved14 February 2021.
  12. ^"Hepatitis A Vaccine Information".Vaccine Information. ImmunizationInfo. Archived fromthe original on 30 June 2007. Retrieved19 June 2008.
  13. ^abcd"Hepatitis A Vaccine: What you need to know"(PDF).Vaccine Information Statement. U.S.Centers for Disease Control and Prevention (CDC). 21 March 2006.Archived(PDF) from the original on 20 November 2007. Retrieved12 March 2007.
  14. ^"Hepatitis, Viral, Type A".Travelers' Health: Yellow Book (CDC). Archived fromthe original on 28 March 2007. Retrieved12 March 2007.
  15. ^ab"Hepatitis A: Introduction". NHS Direct. 10 October 2006. Archived fromthe original on 10 March 2007. Retrieved12 March 2007.
  16. ^Ott JJ, Irving G, Wiersma ST (December 2012)."Long-term protective effects of hepatitis A vaccines. A systematic review".Vaccine.31 (1):3–11.doi:10.1016/j.vaccine.2012.04.104.PMID 22609026.
  17. ^Irving GJ, Holden J, Yang R, Pope D (2012)."Hepatitis A immunisation in persons not previously exposed to hepatitis A".Cochrane Database Syst Rev.7 (7) CD009051.doi:10.1002/14651858.CD009051.pub2.PMC 6823267.PMID 22786522.
  18. ^Patient Information LeafletArchived 20 July 2011 at theWayback Machine, sanofi pasteur, July 2010. Archived on the electronic Medicines Compendium of the UK. Accessed 30 November 2010.
  19. ^EpaxalArchived 19 January 2011 at theWayback Machine, Crucell website. Accessed 30 November 2010.
  20. ^Full Prescribing InformationArchived 18 August 2011 at theWayback Machine, GlaxoSmithKline, July 2010. Archived on FDA website. Accessed 30 November 2010.
  21. ^"VAQTA (Hepatitis A Vaccine, Inactivated)"(PDF). U.S.Food and Drug Administration (FDA). p. 11. Archived fromthe original(PDF) on 21 February 2015. Retrieved7 February 2014.
  22. ^"Twinrix".U.S.Food and Drug Administration (FDA). 3 October 2019. Archived fromthe original on 22 September 2019. Retrieved18 October 2020.
  23. ^"Australian Product Information – Vivaxim (Salmonella typhi Vi polysaccharide and hepatitis A virus antigen) Vaccine". Retrieved18 October 2020.
  24. ^"Vivaxim Salmonella typhi vaccine; Hepatitis A vaccine".NPS MedicineWise. 6 March 2020. Retrieved18 October 2020.
  25. ^"Vivaxim 1mL injection syringe composite pack".Therapeutic Goods Administration (TGA). Archived fromthe original on 19 October 2020. Retrieved18 October 2020.
  26. ^"Summary for ARTG Entry: 82745 Vivaxim 1mL injection syringe composite pack". Therapeutic Goods Administration (TGA). Retrieved18 October 2020.[permanent dead link]

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