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Hepatitis A. Vaccination Offers Long-Term Immunity. The Hepatitis A Virus. The HAV Replication Cycle. Hepatitis A. Transmission is typically by the faecal-oral route: Contamination of food or water Close person-to-person contact Sexual oral-anal contact - PowerPoint PPT Presentation
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Hepatitis A
Vaccination Offers Long-Term Immunity
The Hepatitis A Virus
The HAV Replication Cycle
Hepatitis A
– Transmission is typically by the faecal-oral route:• Contamination of food or water• Close person-to-person contact• Sexual oral-anal contact
Less typically, hepatitis A may be transmitted in body fluids such as blood and saliva .
Symptomatic Ratio in Day - Care Children
“ Clinical illness is rare in children infected in the first year of life , occurs in about one - fourth of
those under the age of 15, and is almost universal in adults .
Gust &Feinstone
1990
Symptoms of Hepatitis A in Children & Adults
Complications of Hepatitis A
• Cholestatic Joundice
• Relapsing Hepatitis
• Fulminant Hepatitis
Hepatitis A: Clinical Characteristics of Patients by Age Group
Clinical Characteristics <1-14yrs 15-39yrs 40+yrs (n=1692) (n=4918) (n=1386)
Jaundice 81.7% 86.8% 70.3%
Hospitalised for Hepatitis 17.1% 32.2% 70.3%
Death as a result of Hepatitis 0.1% 0.3% 2.1%
“As there is no specific treatment for hepatitis A, management is basically Supportive…”
Dr lan D Gust & Dr Sptephen M Feinstone
Highly developed countries , such as japan , Australia , and most parts of North America and Europe , are largely low endemicity regions for hepatitis A
Many residents of these areas have no natyral immunity against hepatitis A virus
Morbidity & Mortality per 100,000 Unprotected Travellers to Developing Countries per Month of
Stay Abroad INFECTION Morbidity Case Fatality rate(%)
Mortality_____________________________________________________________________
_
Malaria,West Africa 2400 2(for p. falciparum) 40Malaria ,South America 50 2(for p. falciparum) 0.15Hepatitis A: generally 300(-600) 0.1 0.3(-0.6) Hepatitis A:backpackers 2000 0.1 2Hepatitis B:expatriates 80(-240) 2 1.6(-4.8)Typhoid fever : usual destination 3 1 0.03Typhoid : India , N-,W-Africa 30 1 0.3Ppliomyelitis : symptomatic 0.1 20 0.02Poliomyelitis: Symptomatic 0.1 20 0.02Poliomyelitis: asymptomatic2(-100) - (contacts)Cholera 0.3 2 0.006
Travellers at Risk of HAV Infection
• Tourists
• Business travellers
• Foreign aid workers
• Airline Personnel
• Missionaries
• Professionals working abroad
“Symptomatic hepatitis A is the most frequently occurring immunisable infection in travellers”
“The incidence rate of symptomatic hepatitis A for a one month journey from an industrialised country to a developing country is 3/1000 for the usual non-immune traveller”
“This applies also to tourists staying in renowned hotels”
Uk Travellers Abroad
Protection is advised for non-immune
Travellers from the UK visiting all countries
Outside of Northern Europe, North America,
New Zealand and Australia
“ In unprotected travellers , hepatitis A occurs 40 times more frequently than typhoid fever and 800 times more frequently than cholera”
Steffen 1991
This availabillity of an effective hepatitis A vaccine will make it possible , at last, to provide protection against one of the oldest disease threats to the healthy soldier
Col WH Bancroft MDWalter Reed Army Institute,washington DC
This enhanced risk of hepatitis Ainfection for the nursing profession … prompts us to demand that (this type of disease) should also of professional diseases
Windorfer et al 1989
Hepatitis A in both employees and household contacts is strongly related to contact with children whoo attend day-care centre
Hadler et al
1980
Protection is advised for close contacts of all ages in order to control outbreaks of hepatitis A in households and in institutions
Joint Committee on
Vaccination and Immunisation
Prevention of Hepatitis A
• Improvement in water Supply, sanitation and hygiene
• Isolation of infected individuals
• Passive immunisation (IG)
• Active immunisation ( vaccination)
Passive Immunisation
• Short –term protection- requires frequent renewal
• No stimulation of antibody production in recipient
• Plasma- derived product
• Large injection volumes
Active Vaccination • Long –term immunity from active
vaccination
• Stimulates antibody production in the recipient
• Non plasma-derived product
• Small IM injection volumes administered via deltoid
Recombinant Vaccines
• HAV epitope is complex
• Current technology has not been able to reproduce the epitope in isolation
• The development of a recombinant vaccine against hepatitis A will be very difficult
Live, Attenuated Vaccines
• Difficult to develop
• Under-attenuation may lead to active infection
• Over-attenuation may lead to vaccine failure
• Re-emergence infection in both recipient and close contacts
Inactivated Vaccine
• Killed virus – incapable of causing active infection
• Killed Virus – possesses the antigens which stimulate the production of
anti-HAV
• Can be developed using proven technology (polio, salk)
‘Havrix’ Hepatitis A Vaccine Seroconversion Rates
Injections given at months o ad 1 with a booster dose at 6 months
Blood Sample Taken
M O N T H
1 2 7
% Seroconversion 95.6 99.9 100
(987/1032) (1035/1036) (592/592)
Hepatitis A
Vaccination Offers Long- Term Immunity
Havrix
Hepatitis A VaccinePrescribing Information and References available at this
meeting
SBSmithkline Beecham
Pharmaceuticals
‘Havrix’ is a trade mark1992 smithkline Beecham Pharmaceuticals
