Best Rate (Hyderabad) Call Girls Jahanuma â 8250192130 â High Class Call Girl...
Â
Hepatitis B Vaccine revisited - Ideal Schedule & recommendations
1. Hepatitis B Immunization : Choosing the
Most Effective Schedule
Dr Gaurav Gupta, MD
Charak Clinics, Mohali.
MAAP, MIAP
1
2. Conflict of Interest
⢠Received grants from various vaccine manufacturers
including
⢠- Sanofi Pasteur
⢠- GSK
⢠- Abbott
⢠- Wyeth etc.
2
3. Scope
⢠The hepatitis burden- Worldwide & India
⢠Hepatitis B â disease profile
⢠What is an ideal vaccination schedule?
⢠Why is 0, 1 & 6 the most effective?
3
4. Global BurdenâHepatitis B Virus Infection
⢠2 billion people infected with HBV
⢠> 350 million have chronic HBV infection
⢠>40 million in India
⢠600,000 HBV-related deaths
⢠93% of deaths were the result of chronic infection
⢠88% of the world's population live in areas where the
prevalence of chronic HBV infection is high (>8% HBsAg +) or
moderate (2-7% HBsAg +)
Scaling up Global Access to Hepatitis B Vaccination. WHO July 2009 4
5. Leading Causes of Infectious Disease
Deaths Worldwide
Disease Est. Deaths per Year
Lower respiratory tract infections ~4.2 million
Diarrheal diseases ~2.2 million
HIV/AIDS ~2.0 million
Tuberculosis ~1.5 million
Hepatitis viruses ~1 million
Hepatitis B virus ~620,000
Hepatitis C virus ~366,000*
Malaria ~900,000
Pertussis ~295,000
Neonatal tetanus ~213,000
Measles ~197,000
Source: WHO, UNICEF, Perz et al, J Hepatology, 2006 5
8. Three distinct levels of Hepatitis B endemicity
Hepatitis B seroprevalence (Hadler& Margolis)
Endemicity Area HBsAG Infected Adults Regions Transmission
Seroprevalence
Asia (except Japan and â˘Vertical
India), Africa, most of â˘Horizontal
Middle East, the Almost all infections are
High >8% >70% Amazon basin of south acquired in infancy or
America, most pacific early chidlhood, and few
Island groups and adults remain
Maoris susceptible to infection
India, part of the Middle Mixed and
East, Western Asia, transmission occurs in
Japan, Eastern & all age groups but
Southern Europe, and predominant period of
Intermediate 2% - 8% 20% - 50% most south & Central transmission probably
America occurs among young
children, adolescents
and young adults.
USA, Canada, Western Primarily among adults
Europe, Australia and Nevertheless,
New Zealand transmission during the
perinatal period and
Low <2% <20% during childhood
provides a significant
contribution to the HBV
carrier burden
8
14. Risk of acquiring HBV from a needlestick
Source-HBs Ag positive, HBe Ag negativeâ1-6%
Source-HBs Ag positive, HBe Ag positive---22-40%
HCV-3-10%, HIV-0.2-0.5%
14
16. HBV Vaccination â Fast Facts
1. Plasma derived vaccines â 1982
2. Yeast derived vaccines â 1986
3. First Mass immunization program â Taiwan 1984
4. Most commonly used vaccination â more than 1 billion doses
given
5. First vaccination to prevent cancer
16
17. Success of Hepatitis B vaccine
⢠The vaccine has an outstanding record of safety and
effectiveness.
⢠Vaccination has excellent effectiveness - reduced the rate of
chronic infection to less than 1% from 8-15 %
⢠In 2009, 177 countries included the hepatitis B vaccine into
their national scheduleď major increase compared with 31
countries in 1992, when WHO passed a resolution
recommending global vaccination against hepatitis B
17
Dr. Gaurav Gupta, Charak Care Clinics, Mohali
18. Questions needed to be asked regarding Ideal
Schedule for Hep B vaccine?
1. Has it been used for extensive period of time?
2. Does it protect the highest âat riskâ population?
3. Are there enough evidence regarding its effectiveness?
4. Are other countries using the same in their National
Schedules?
5. Can it be piggy-backed on to the National Schedule in our
Country?
18
19. Hepatitis B immunization
Birth dose and interval between the doses are extremely
important :
⢠not only for the robustness of the immune
response, but
⢠as well for the prevention of vertical and horizontal
transmission and
⢠the long term protection post-vaccination.
19
20. Importance of vaccination schedule at 0-1-6 mo/o
vs 2-4-6 mo/o.
Results: Anti-HBs Post-dose 3
Group 1 Group 2
Hep.B at 0-1-6 Hep.B at 2-4-6
100% 99.0%
Anti-HBs ⼠10 mIU/mL
[97.2 ; 100] [94.3 ; 99.4]
3 643 mIU/mL 1 052 mIU/mL
GMTs
[502;709] [163;253]
Post-dose 2 (at 2 months of age): Anti-HBs ⼠10 mIU/mL in
47% of infants of group 1 versus only 9% in group 2
Greenberg D et al.- Ped. Inf. Dis. Journal. 21(8):769-776, August 2002
20
21. Ab titres (ShanvacB) with 0-1-2 &0-1-6 schedules
7000
6375.86
6000
5000
GMT (mIU/ml) 0,1,2 schedule
GMT (mIU/ml) 0,1,6 schedule
GMT (mIU/ml)
4000
3000
2000
1000 749.12
41.7 23.44 84.39 79.70
0
After 1st dose After 2nd dose After 3rd dose
GMT (mIU/ml)
21
22. GMT in infant vaccinated against Hepatitis B by
different vaccination schedules
22
23. WHO targets hepatitis B control in Western
Pacific Region
An universal vaccination program was launched in Taiwan in
1984
HBsAg positive rate in children < 12 y/o :
⢠Before vaccination program: 9.8%
⢠After the institution of program,
â 4.8% at 5 years
â 1.3% at 10 years
â 0.7% at 15 years
The annual rate of incidence of childhood HCC decreased
from 0.52 to 0.13 per 100 000 children after the vaccination
program.
The schedule implemented is birth, 1 and 6 months of age.
23
24. Estimation of annual incidence of HBs Ag chronic carrier
due to vertical transmission
ďˇ What is the ÂŤcostÂť of a delayed schedule?
Total Annual
incidence of
Universal HBsAg+ HBeAg Estimated chronic
prevention Mothers + Infected Rate per carriage due
of vertical % mother neonates 100 000 to vertical
transmissi s (%) Births transm
on (Yes/ %HBsA per year*
No) g+
India (1996) No 4.6 18.0 0.67 605 162 563
Singapore Yes 3.4 39.0 0.92 827 474
(1998)
Bangladesh No 3.5 30.2 0.76 687 25 690
Chauvin P, Ekra D, Plotkin S.- Vaccine. 2002 Jul 26;20(23-24):2848-50
24
26. The Rationale
1st Dose â At birth - Prevents vertical transmission
2nd Dose â Min 4 wk later â Limited number of seroconversion
after 1st dose, hence closely spaced second dose â prevents
immediate horizontal transmission
3rd Dose -- Min 8 weeks after 2nd Dose,
-- Min 16 weeks after 1st Dose,
-- After 24 weeks age,
(ACIP/ AAP recommendations)
Leads to increased antibody titres â Better Long Term protection
26
27. AAP recommendations - hepatitis B, 2012
⢠Administer Monovalent HepB to all newborns before hospital discharge
⢠The second dose should be administered at age of 1 to 2 months
⢠The final dose should be administered no earlier than age 24 weeks
27
Dr. Gaurav Gupta, Charak Care Clinics, Mohali
28. Comparision of vaccination schedule in
different countries throughout world
Country Hepatitis B vaccination schedule
USA birth; 1-2, 6-18 months;
Canada 1st contact; +1, >+2 months;
England birth; 1, 2, 6 months;
Germany 2, 4, 11-14 months;
South Africa 6, 10, 14 weeks;
Australia birth; 2, 4, 6 months; 1, 10-13 years;
India Birth; 6, 10, 14 weeks;
China birth; 1, 6 months;
Ref: WHO. Immunization surveillance, assessment and monitoring
Available at:http://www.who.int/immunization_monitoring/data/data_subject/en/index.html
28
29. International Schedules
Majority of schedules begin at birth
Many vaccination schedules end at 6 months age or more
Gap of at least 8 weeks between 2nd and 3rd doses
If the gap is less, then a 4th dose given
29
30. Key Points
⢠The GMTs with 0, 1, and 6 months schedule are upto 10
times higher than 0, 1, and 2 months schedule.
⢠Infants who achieve higher Anti HBs titers maybe
protected better in later years.
⢠The seroprotection rates are found to be highest when
the interval between the second and third dose is longer.
⢠The classic 0, 1, and 6 months schedule yields a high
seroconversion rate and relatively high titers of anti-HBs
that will persist for an extended period of time.
30
31. IAP recommendations
Hep B vaccine may be given in any of the following schedules:
(i) Birth, 1 and 6 months
(ii) Birth, 6 and 14 weeks
(iii) 6, 10 and 14 weeks
(iv) Birth, 6 weeks, 6 months
(v) Birth, 6 weeks,10 weeks, 14 weeks
The IDEAL schedule is 0 1 6 months.
31
32. 0, 1 & 6 months
⢠Gold standard,
⢠Protects high risk infants,
⢠Enough evidence regarding long term efficacy (at least 25
years), and being used by many countries,
⢠Cannot be easily integrated with the national schedule
IAPCOI â Most widely used, IDEAL, High Antibody Titres
32
33. 0, 6 & 14 weeks
â˘Not enough evidence regarding long term effectiveness
â˘Protects High risk infants,
â˘Can be piggy backed to existing EPI
â˘Slightly lower titres since 3rd dose completed before 24 weeks
- ? Clinical significance
IAPCOI â Recommended for Public Health since protects
against Vertical Transmission, and can be integrated with EPI
33
34. 6,10 & 14 weeks
â˘Does NOT protect against vertical transmission
â˘Can be piggybacked to EPI,
IAPCOI â Only recommended for missed birth dose
34
35. Birth, 6,10 & 14 weeks
â˘Protects against vertical transmission
â˘Can be piggybacked to EPI,
â˘Increases overall cost of vaccination
35
36. Birth 6 weeks & 6 months
Similar to the classic schedule of 0 1 & 6 months
Can be partially piggybacked to EPI,
IAP recommendation for Office Practice ?
0, 4/6 week, 6 months
36
37. Interesting facts â IAPCOI recommendations
â˘Catch-up vaccination schedule - 0,1 & 6 months for ALL
children to prevent horizontal transmission.
â˘For management of infants of HbsAg +ve mothers - the âclosely
spaced scheduleâ should NOT be used.
37
38. Importance of a 6 month visit: pediatricians perspective
⢠24 wk (6 mo) visit introduces a potential visit between
14 weeks (DTP3) and 36 weeks (measles) to
evaluate child development and monitor progress
including
⢠Major motor skills
⢠Fine motor skills
⢠Language
⢠Vision and hearing
⢠Social achievements and play
⢠Evaluation of weaning issues
38
39. FAQ
When should double dose be given?
In elderly, immunocompromised and chronic renal
failure patientsâ 4 doses at 0,1,2 and 12 months,
double dose is to be given
Should routine testing of HBs Ab be done after
completion of vaccination schedule ?
Only for a small minority of vaccinees including babies
of HBsAg +ve mothers, close contacts of HbsAg +ve,
health care workers and people with co-morbidities,
39
40. FAQ
What antibody titres signify a response?
Antibody levels more than 10 mIu/ml signify a response
What should be done in Nonresponders?
Non responders should be tested for Hepatitis B carrier
status. If negative, repeat the complete vaccination
schedule, 50% would respond , rest are permanently
susceptible
40
41. FAQ
Is booster dose required ?
⢠Routine boosters are NOT needed in healthy children and
adults
⢠Individuals who respond to the vaccination series and have
levels of 10 mIU/ml after vaccination are protected against
hepatitis B disease for life even if the levels drop to below
protective levels or are undetectable later. This is due to
Immune memory.
⢠In immunocompromised and those who have CRF, CLD etc.
levels should be regularly checked (? Yearly) and booster
dose given when the levels fall below protective levels
41
42. FAQ
What the accelerated schedules for HBV vaccine?
⢠0, 1, 2 & 12 months
⢠0, 7 days, 21 days and 12 months
What are the recommendations for premature babies?
⢠Some infants born prematurely with low birth weight (<2000 g)
may not respond well to vaccination at birth. However, by one
month of chronological age, all premature infants, regardless
of initial birth weight or gestational age, are likely to respond
adequately.
⢠Give birth dose, but donât count it. Start afresh from1 month
age
42
43. Longer needle length for Hep-B vaccination of
macrosomic neonates
⢠Use of a longer (1 in.) rather than a standard (5/8 in.) needle
used for macrosomic neonates (birthweight over 4000 g) may
affect antibody titers
⢠Fifty nine healthy infants were vaccinated at birth, 1, and 6
months of age with hepatitis B vaccine,
⢠Macrosomic infants who were immunized with a longer needle
achieved significantly higher antibody titers to hepatitis B
surface antigen than standard needle length (median, 3890.2
vs 1311.7 mIU/mL)
Ref: Vaccine, Volume 30, (21), 2 May 2012, 3155â58
43
I am sure that most of you sitting in this room are already convinced that HB is a major public health problem But just in case there is someone who isn't, and because this is the first talk on this meeting, let's review the tremendous burden of this disease. An estimated 2 billion people have been infected with HBV More than 350 million have chronic HBV infection Approximately 88% of the world's population live in areas where the prevalence of chronic HBV infection is high or moderate (as defined by the prevalence of HB surface antigen) There were ~ 600,000 HBV-related deaths in 2002 Approximately 93% of these deaths were the result of chronic infection