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MAN BAHADUR RANA
BPH,ACAS,NEPAL
- HBV is a complex 42 nm double shelled
particle.
- The outer surface or envelope of virus
contains Hepatitis B surface antigen ( HBsAg).
- It encloses an inner icosahedral 27nm
nucleocapsid (core), which contain hepatitis B
core antigen (HBcAg).
- Inside the core is the genome, a circular
double stranded DNA and a DNA polymerase.
1. HBsAg:
- Surface antigens (envelope protein).
- It is made up of lipid, protein and
carbohydrate.
2. HBcAg :
- It is the core(nucleocapsid) antigen of the
virus
- It is not detectable in patients blood.
3. HBeAg:
- It appears in serum along with HBsAg but
disappears within a few weeks.
- HBcAg and HBeAg though
immunologically distinct are coded by the
same gene.
There are three important modes of transmission
of HBV infection.
1. Parenteral
2. Perinatal
3. Sexual
Parenteral:
- Transmission of infection may result from
accidental inoculation of minute amounts of
blood, blood products or fluid containing HBV
during medical, surgical or dental procedure.
- Needlestick injuries, use of contaminated
needles and syringes, intravenous and
percutaneous drug abuse, ear and nose
piercing, tattooing, acupuncture, sharing of
shaving razor and kissing can transmit HBV
infection.
Perinatal:
- Transmission probably occurs when
carrier mothers blood contaminates the
mucous membranes of the new born during
birth.
Sexual Transmission:
- HBV is present in body fluids such as
semen and vaginal secretions, hence it can be
transmitted by sexual contact.
- Male homosexual are at higher risk of
acquiring infection.
Clinical features:
- The incubation period varies from 6 weeks
to 6 months.
- The course of acute HBV infection can be
divided into three phase.
. Pre-ecteric
. Icteric
. Convalescent
Pre-icteric phase:
In this phase patient develops malaise,
anorexia, weakness, nausea and vomiting
Icteric phase:
Patient develops jaundice, pale stools,
and dark urine.(bilirubinuria).
Convalescent phase:
This phase is long and drawn out with
malaise and fatigue.
1. Laboratory diagnosis of HBV infection can
be carried out by detection of hepatitis B
antigen and antibodies.
These can be detected by sensitive and
specific tests like ELISA and RIA.
2. Viral DNA Polymerase:
It appears transiently in serum during pre-
icteric phase.
3. Polymerase chain infection:
HBV DNA level can be detected in serum
by PCR . It is a highly sensitive test.
Biochemical test:
- SGPT and SGOT level increases
- Serum bilirubin level indicates the degree
of jaundice and may rise up to 25 fold.
- General Preventive Measure
- Immunisation
General Preventive Measure:
 These include health education ,
improvement of personal hygiene.
 Use of unsterile needle, syringes and other
material must be avoided to prevent hepatitis
B infection.
i) Passive immunization:
- Passive immunization may be employed
following any accidental exposure to hepatitis B
infection.
- It can be given in doses of 300-500 IU
intramuscularly.
- Vaccine should be administered as early as
possible after exposure, preferably with in 48
hours.
- A second dose is given at an interval of 4
weeks, after the first dose.
- It may not prevent infection but protect
against illness and the development of carrier
state.
ii) Active immunization:
Following vaccines are available
a) Plasma derived vaccine
b) Recombinant yeast hepatitis B Vaccine.
a) Plasma derived vaccine:
- It consist of purified 22nm particles of
HBsAg, prepared from the plasma of
symptomless carriers.
- The particles are seperated by
ultracentrifugation and treated with
proteinase, 8M urea and formaldehyde.
- This vaccine is still being produced and
used particularly in developing countries
where the need is greatest.
b) Recombinant yeast hepatitis B Vaccine:
 It is produced by cloning the HBsAg gene in
yeast Saccharomyces cerevisae and the HBsAg
particles produced are extracted and purified
for use as vaccine.
 This vaccine is safe, antigenic, free from
side effects and as immunogenic as plasma
derived vaccine.

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Hepatitis b virus

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  • 5. - HBV is a complex 42 nm double shelled particle. - The outer surface or envelope of virus contains Hepatitis B surface antigen ( HBsAg). - It encloses an inner icosahedral 27nm nucleocapsid (core), which contain hepatitis B core antigen (HBcAg). - Inside the core is the genome, a circular double stranded DNA and a DNA polymerase.
  • 6. 1. HBsAg: - Surface antigens (envelope protein). - It is made up of lipid, protein and carbohydrate. 2. HBcAg : - It is the core(nucleocapsid) antigen of the virus - It is not detectable in patients blood.
  • 7. 3. HBeAg: - It appears in serum along with HBsAg but disappears within a few weeks. - HBcAg and HBeAg though immunologically distinct are coded by the same gene.
  • 8. There are three important modes of transmission of HBV infection. 1. Parenteral 2. Perinatal 3. Sexual Parenteral: - Transmission of infection may result from accidental inoculation of minute amounts of blood, blood products or fluid containing HBV during medical, surgical or dental procedure.
  • 9. - Needlestick injuries, use of contaminated needles and syringes, intravenous and percutaneous drug abuse, ear and nose piercing, tattooing, acupuncture, sharing of shaving razor and kissing can transmit HBV infection. Perinatal: - Transmission probably occurs when carrier mothers blood contaminates the mucous membranes of the new born during birth.
  • 10. Sexual Transmission: - HBV is present in body fluids such as semen and vaginal secretions, hence it can be transmitted by sexual contact. - Male homosexual are at higher risk of acquiring infection.
  • 11. Clinical features: - The incubation period varies from 6 weeks to 6 months. - The course of acute HBV infection can be divided into three phase. . Pre-ecteric . Icteric . Convalescent
  • 12. Pre-icteric phase: In this phase patient develops malaise, anorexia, weakness, nausea and vomiting Icteric phase: Patient develops jaundice, pale stools, and dark urine.(bilirubinuria). Convalescent phase: This phase is long and drawn out with malaise and fatigue.
  • 13. 1. Laboratory diagnosis of HBV infection can be carried out by detection of hepatitis B antigen and antibodies. These can be detected by sensitive and specific tests like ELISA and RIA. 2. Viral DNA Polymerase: It appears transiently in serum during pre- icteric phase.
  • 14. 3. Polymerase chain infection: HBV DNA level can be detected in serum by PCR . It is a highly sensitive test. Biochemical test: - SGPT and SGOT level increases - Serum bilirubin level indicates the degree of jaundice and may rise up to 25 fold.
  • 15. - General Preventive Measure - Immunisation General Preventive Measure:  These include health education , improvement of personal hygiene.  Use of unsterile needle, syringes and other material must be avoided to prevent hepatitis B infection.
  • 16. i) Passive immunization: - Passive immunization may be employed following any accidental exposure to hepatitis B infection. - It can be given in doses of 300-500 IU intramuscularly. - Vaccine should be administered as early as possible after exposure, preferably with in 48 hours. - A second dose is given at an interval of 4 weeks, after the first dose.
  • 17. - It may not prevent infection but protect against illness and the development of carrier state. ii) Active immunization: Following vaccines are available a) Plasma derived vaccine b) Recombinant yeast hepatitis B Vaccine.
  • 18. a) Plasma derived vaccine: - It consist of purified 22nm particles of HBsAg, prepared from the plasma of symptomless carriers. - The particles are seperated by ultracentrifugation and treated with proteinase, 8M urea and formaldehyde. - This vaccine is still being produced and used particularly in developing countries where the need is greatest.
  • 19. b) Recombinant yeast hepatitis B Vaccine:  It is produced by cloning the HBsAg gene in yeast Saccharomyces cerevisae and the HBsAg particles produced are extracted and purified for use as vaccine.  This vaccine is safe, antigenic, free from side effects and as immunogenic as plasma derived vaccine.