Viral Hepatitis: A, B, C, D, E

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Viral Hepatitis: A, B, C, D, E

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Title: Viral Hepatitis: A, B, C, D, E

1
Viral Hepatitis A, B, C, D, E
Wayne A. Duffus, MD, PhD November 2nd, 2009
2
Viral Hepatitis - Historical Perspective
Enterically transmitted
Infectious
A
E
NANB
Viral hepatitis
Parenterally transmitted
B
D
C
Serum
F, G, ? other
3
Viral Hepatitis
A
B
C
D
E
Source of
feces
blood/
blood/
blood/
feces
virus
blood-derived
blood-derived
blood-derived
body fluids
body fluids
body fluids
Route of
fecal-oral
percutaneous
percutaneous
percutaneous
fecal-oral
transmission
permucosal
permucosal
permucosal
Chronic
no
yes
yes
yes
no
infection
Prevention
pre/post-
pre/post-
blood donor
pre/post-
ensure safe
exposure
exposure
screening
exposure
drinking
immunization
immunization
risk behavior
immunization
water
modification
risk behavior
modification
4
Viral Hepatitis 1982-1993
34
42
16
3
Source CDC Sentinel Counties Study on Viral
Hepatitis
5
Estimates of Acute and Chronic DiseaseBurden for
Viral Hepatitis, United States
HAV
HBV
HCV
HDV
Acute infections
(x 1000)/year
125-200
140-320
35-180
6-13
Fulminant
deaths/year
100
150
?
35
Chronic
0
1-1.25
3.5
infections
million
million
70,000
Chronic liver disease
deaths/year
0
5,000
8-10,000
1,000
Source CDC -Range based on estimated annual
incidence, 1984-1994.
6
Hepatitis A Virus (HAV)
7
HAV Transmission

Close personal contact
household contact, sex contact, child day care
centers
Contaminated food, water
infected food handlers, raw shellfish
Blood exposure (rare)
injecting drug use, transfusion

8
Hepatitis A - Clinical Features

Incubation period Mean 30 days Range 15-50
days
Jaundice by lt6 yrs, lt10 age group 6-14
yrs 40-50 gt14 yrs 70-80
Complications Fulminant hepatitis Cholestati
c hepatitis Relapsing hepatitis
Chronic sequelae None

9
HAV - Typical Serologic Course
Symptoms
Total anti-HAV
ALT
Titer
Fecal HAV
IgM anti-HAV
4
5
6
12
24
0
1
2
3
Months after Exposure
10
Serological Testing

HAV total Ab appears 4-5 weeks after infection
and remains positive for the patients lifetime
HAV IgM is present at the onset of symptoms and
usually disappears after 4-6 months.
The presence of total Ig without IgM indicates
past infection

11
HAV Immune Globulin

IM administration within 2 weeks after HAV
exposure is gt85 effective in preventing
symptomatic infection.
HAV IG and vaccine does not alter seroconversion
rates but lower serum antibody concentrations may
be obtained.
HAV IG administration will alter normal
serological profiles for 6-12 months.

12
Hepatitis A Virus

Highest virus concentrations occur in stool 1-2
weeks before the onset of illness. Transmission
is most likely at this time.
Minimal virus present in stool 1 week after the
onset of jaundice.
In neonates and young children, virus may be
detected in stool for months.

13
Virus Detection

Culture is worthless except for research
purposes.
PCR detection is available but cannot distinguish
recent from past infection.
Nucleic acid sequencing is useful for tracking
HAV outbreaks.

14
Mitch, a 43 year old salesman, has increasing
fatigue x 5 days and vague abdominal pain x 3
days. He ate at the Stage Deli (site of a recent
HAV outbreak) 10 days previously. His liver
enzymes are within normal limits.

HAV AB (total) Positive
HAV IgM Negative

Does he have HAV infection?
15
CDC RecommendationsTesting and Vaccination
16
PRE-VACCINATION TESTING

Considerations
Cost of vaccine
Cost of serologic testing (including visit)
Prevalence of infection
Impact on compliance with vaccination
Likely to be cost-effective for
Persons born in high endemic areas
Older U.S. born adults
Older adolescents and young adults in certain
groups(e.g., Native Americans, Alaska Natives,
Hispanics, IDUs)

17
POST-VACCINATION TESTING
Not recommended

High response rate among vaccinees
Commercially available assay not sensitive enough
to detect lower (protective) levels of
vaccine-induced antibody

18
ACIP RECOMMENDATIONSPERSONS AT INCREASED RISK
OF INFECTION

Men who have sex with men
Illegal drug users
International travelers
Persons who have clotting factor disorders
Persons with chronic liver disease

19
STD Treatment GuidelinesMMWR August 4, 2006 55
(RR11)
Vaccination against hepatitis is the most
effective means of preventing sexual
transmission of hepatitis A and B.
20
Indications for IG for Post-Exposure Prophylaxis

Household and sexual contacts if exposure is
within 2 weeks.
Childcare center employees and children when HAV
infection is identified in a child or employee.
Close school contacts if transmission within the
school has occurred.

21
Indications for IG for Post-Exposure Prophylaxis

Person exposed to contaminated food/water.
Persons who ate food prepared by HAV food
handler.

22
Hepatitis A Surveillance and Response
23
Hepatitis A Surveillance Response

Urgently reportable condition in S.C. Acute HAV
infection must be reported by phone to health
department within 24 hours.
Investigation of a case of hepatitis A must be
initiated by health department and district epi
staff within 24 hours of notification.
All cases must be reported to CDC.

24
Important Information

Date of onset of symptoms
Occupation
If child, whether child attends childcare
Names of household/sexual contacts
Restaurants attended 2-6 weeks prior to symptoms

25
Management of Outbreaks

Initiate enteric precautions during the first 2
weeks of illness.
Refer symptomatic contacts to physician.
Exclude adults/children with HAV infection from
work/school until 1 week after onset of illness
or until IG PEP has been initiated.
Provide education re transmission, prevention,
and hygiene.

26
Hepatitis E Virus
27

Amita, a 23 year old student, returned from India
one month ago where she spent 3 weeks visiting
her future in-laws. She presented with fever,
jaundice, malaise, and significantly elevated ALT
levels. Antibody tests were positive for HEV IgG
and IgM.

How does she prevent the spread of HEV to family
and friends?

28
Hepatitis E Virus

Most outbreaks associated withfecally
contaminated drinking water
Minimal person-to-person transmission
U.S. cases usually have history of travelto
HEV-endemic areas

29
Geographic Distribution of Hepatitis E
Outbreaks or Confirmed Infection in gt25 of
Sporadic Non-ABC Hepatitis
Source CDC
30
Hepatitis E Virus

Incubation period Average 40 days Range
15-60 days
Case-fatality rate 1-3 overall 15-25
in pregnancy
Illness severity Increased with age
Chronic sequelae None identified

31
Typical Serological Course - HEV
Symptoms
anti-HEV
ALT
IgM anti-HEV
Titer
Virus in stool
0
1
2
3
4
5
6
7
8
9
10
11
12
13
Weeks after Exposure
32
Serological Profile

HEV IgM is usually present at the onset of
symptoms and persists for 3-4 months
HEV IgG is also present at the onset of symptoms
and persists for the patients lifetime

33
CDC Criteria for Testing Acute Phase Sera

Discrete onset of illness with jaundice or
Serum ALT gt2.5 times the upper limit of normal
and
HAV IgM negative
HBV Core IgM negative
HCV Ab negative

34
HEV Detection

Culture is worthless
PCR can detect HEV RNA in serum and stool
specimens from 2 weeks before, to 2 weeks after,
the onset of symptoms
Nucleic acid sequencing is useful for tracking
HEV outbreaks

Steps to prevent HEV transmission in home
setting?
Safe sex practices
Do not share eating/grooming utensils.
Respiratory precautions
Vigorous hand washing
No special requirements needed

36
Hepatitis C Virus
37

Claudia is a 46 year old divorced female.
She has a new man in her life.
She has had unprotected sex for the past 3 weeks.
She just learned that her new friend is HCV
positive.
What is her HCV risk?

38
What is Claudias Risk of Infection?

High risk HCV can be transmitted sexually.
Low risk The efficiency of sexual transmission
is low.

39
HCV - Sources of Infection
Injecting drug use 60
Sexual 15
Transfusion 10 (before screening)
Other 5
Unknown 10
Nosocomial Health-care work Perinatal
Source Centers for Disease Control and Prevention
40
Sexual Transmission

Transmission efficiency is low
Rare between long-term steady partners (1.5)
Factors that facilitate transmission between
partners (e.g., viral load) are unknown
Male to female transmission may be more
efficient

41
Other Transmission Issues

HCV is not spread by kissing, hugging, sneezing,
coughing, food or water, sharing eating utensils
or drinking glasses, or casual contact
HCV infection status should not be used to
exclude patients from work, school, play,
child-care or other settings

42
Hepatitis C Genotypes

Genotype Countries Where Prevalent
1a USA, England, Europe
1b USA, Japan, Europe
2a, 2b, 2c, 2d Japan, China
3a, 3b, 3c, 3d, 3e, 3f Scotland, England
4a, 4b, 4c, 4d, 4e, 4f,
4g, 4h, 4i, 4j Middle East, Africa
5a Canada, South Africa
6a Hong Kong, Macau

43
Genotype Distribution
44
Hepatitis C A Global Health Problem
170 Million Carriers Worldwide, 3-4 MM new
cases/year
EAST MEDITERRANEAN 20M
WEST EUROPE 9 M
FAR EAST ASIA 60 M
U.S.A. 4 M
SOUTH EAST ASIA 30 M
AFRICA 32 M
SOUTH AMERICA 10 M
AUSTRALIA 0.2 M
SOURCE, WHO 1999
45
Acute Hepatitis C Clinical Presentation and
Natural History

HCV RNA can be detected in blood within 1-3 weeks
after exposure
Average time from exposure to seroconversion is
8-9 weeks
Average time from exposure to symptoms period 6-7
weeks
Liver injury (elevations in ALT) with 4-12 weeks
Symptoms develop in only of 20 of patients
Nonspecific 10-20
Jaundice in only 20-30

CDC. MMWR. 1998 47(No. RR-19)1-39. Hoofnagle
JH Hepatology. 199726 (suppl 1) 15S-20S NIH
Consensus Development Conference Panel Statement
Management of Hepatitis C, 2002
46
Hepatitis C Infection

Incubation period Average 6-7 weeks
Range 2-26 weeks
Case fatality rate Low
Chronic infection 75-85
Chronic hepatitis 70 (most asx)
Cirrhosis 10-20
Mortality from CLD 1-5

47
Natural History of Hepatitis C
Acute Hepatitis C
10-20 years
Chronic Hepatitis 75-85
Cirrhosis 20
Hoofnagle JH Hepatology. 199726 (suppl 1)
15S-20S Di Bisceglie, Hepatology, 2000
48
Natural History of Hepatitis C
Annual rate
Hoofnagle JH Hepatology. 199726 (suppl 1)
15S-20S Di Bisceglie, Hepatology, 2000
49
Acute HCV Infection with Recovery
HCV Ab
Symptoms /-
HCV RNA
Titer
ALT
Normal
2
3
4
5
6
1
2
3
4
0
1
Years
Months
Time after Exposure
50
Chronic Hepatitis C

A leading cause of cirrhosis in the US
10,000-20,000 deaths/yr
This number expected to triple in the next 10 to
20 years (without therapy)
Associated with an increased risk of liver cancer
Most common reason for liver transplantation in
the United States

CDC. MMWR. 1998 47(No. RR-19)1-39.
NIH Consensus Development Conference Panel
Statement Management of Hepatitis C, 2002
51
Acute HCV Infection with Progression to Chronic
Infection
HCV Ab
Symptoms /-
HCV RNA
Titer
ALT
Normal
0
1
2
3
4
5
6
1
2
3
4
Years
Months
Time after Exposure
52
Hepatitis C Complications

Hepatitis encephalopathy if untreated can lead
to
Confusion
Disorientation
Hallucination
Stupor/Coma
Jaundice
Pruritus
Renal damage/failure
Hypo/Hyperthyroidism
Varices of Esophagus, Stomach, Rectum
Muscle Wasting

53
Extrahepatic Manifestations of Hepatitis C

Hematologic Mixed cryoglobulinemia
(1025 of HCV patients)
Renal Glomerulonephritis
Dermatologic
Porphyria cutanea tarda
Cutaneous necrotizing vasculitis
Lichen planus

Management of Hepatitis C. NIH Consensus
Statement, 2002.
54
Chronic Hepatitis C Factors Promoting
Progression or Severity

Increased alcohol intake
Age gt 40 years at time of infection
HIV co-infection
Other
Male gender
Chronic HBV co-infection

Claudia needs to see her family physician.
She wants to be tested for HCV.
What test do you recommend?

56
Diagnostic Tests for HCV

Anti-HCV
RIBA (supplemental assay)
Qualitative PCR
Quantitative PCR
Genotyping assays

57
HCV Antibody Tests

Screening tests - total antibody detected
Sensitivity is about 95
Predictive value
High Risk Population 90-95
Low Risk Population 50-60 (false positives)
False Negatives due to window period and
immunosuppression

58
Hepatitis C Antibody TestSignal to Cut Off
(S/CO) Ratio

S/CO ratio is a comparison of the pts positive
EIA result with the labs positive EIA control.
A positive EIA test with a s/co ratio of 3.8 or
higher is indicative that the pt truly has HCV
and that the RIBA test will be positive (95-97
predictive value).

59
HCV RIBA Tests

Used to resolve possible false positive anti-HCV,
particularly in low-risk patients (blood donors)
Use is analogous to HIV western blot

Core
E1
E2/NS1
NS2
NS3
NS4
NS5
5 UTR
60
HCV Screening Algorithm
Negative (non-reactive)
STOP
EIA for Anti-HCV
Positive (repeat reactive)
OR
Negative
RT-PCR for HCV RNA
RIBA for Anti-HCV
Negative
Positive
Positive
Indeterminate
STOP
Additional Laboratory Tests (e.g. PCR, ALT)
Medical Evaluation
Negative PCR, Normal ALT
Positive PCR, Abnormal ALT
Source MMWR 199847 (No. RR 19)
61
Diagnosis of Viral Hepatitis in the Primary Care
Setting Patients Who Have Risk Factors

A single normal ALT level does not rule out
chronic viral hepatitis
ALT levels may be intermittently normal in a
significant number of patients who have chronic
hepatitis C

62
Diagnosis of Chronic Viral HepatitisSerologic
Testing

Patients should be tested if they
Have known risk factors for viral hepatitis
Indicate possible risk factors for hepatitis
Have elevated liver enzymes

Management of Hepatitis C. NIH Consensus
Statement, 1997.
63
Liver Biopsy

May be guided by CT or ultrasound
Provides information regarding
Degree of inflammation
Disease severity
Tissue damage
Presence/absence of cirrhosis
Helps determine
Degree of disease progression
Cause of liver disease
Need for treatment

64
Histologic Staging
65
Diagnostic Evaluation of HCV Infection
66
Hepatitis C Screening and Diagnosis Summary

Suspect disease on the basis of risk factors, not
symptoms
Positive anti-HCV result indicates current
infection until refuted
Measurement of HCV RNA may be required to
establish diagnosis in selected cases

67
Treatment
68
Treatment for Hepatitis C

Interferon Ribavirin x 6-12 months about 40
- 50 sustain viral clearance gt 3 years.
Predictive Factors for Treatment Response
Genotype 2 and 3
Low initial viral load levels
Young age
Low Fibrosis Score (Liver Biopsy)
Female

69
Treatment Side Effects

Depression
Sleep Disturbances (Insomnia)
Irritability
Anger
Psychosis
Excessive Fatigue
Nausea/Diarrhea/Decreased Appetite/Weight Loss
Anemia/Neutropenia
Autoimmune Disorders, especially Thyroiditis
Decreased Libido
Menstrual Irregularities

70
Rationale for the development of a once-weekly
pegylated interferon ?-2b

71
Rationale for Pegylation of Protein
Pharmaceuticals

Pegylation binding of ethylene oxide polymers
to drug molecule
Decreases clearance
Prolonged half-life
Sustained blood levels
Decreases proteolysis
Decreases immunogenicity

Youngster S, et al. Curr Pharm Des.
2002899.Harris JM, et al. Clin Pharmacokinet.
200140539.
72
Why PEG as a Protein-Modifying Agent?

Inert
Water soluble
Can be made any size and shape

Bailon et al., Bioconjugate Chemistry, 2001 Wyss
et al., Current Pharmaceutical Design, 2002
73
Pegylation Effects on Half-life
Longer Shorter
PEG Molecular Weight (PEG size)
The clinical relevance of this in vitro data has
not been established.
Adapted from Youngster et al., Current
Pharmaceutical Design, 2002, 82139-215
74
Pegylation Antiviral Activity
More Less
PEG Molecular Weight (PEG size)
Adapted from Grace M et al., AASLD 2003,
Abstract 1928
The clinical relevance of this in vitro data has
not been established.
75
Relationship between PEG size and Renal Clearance
Wyss et al., Current Pharmaceutical Design,
2002 Xian-Hui He et al., Life Sciences, 1999
76
HCV-Positive Persons for Whom Treatment is
Recommended

Persistently elevated liver enzyme (ALT) levels
Presence of ? HCV RNA (viral load)
A liver biopsy indicating fibrosis or at least
moderate inflammation and necrosis
Cessation of continuing alcohol/substance use
HCV HIV coinfection especially difficult
Goal Clear HCV, restore LFT, reverse
pathology

77
Predicting Response to Treatment
78
Response Rate to Treatment Based on Genotype

Genotype Response Rate
1a/1b 41 of patients
2-6 75 of patients
Overall Response 52 of patients

79
HCV Kinetics
80
Goals of HCV Therapy

Primary HCV RNA below limits of detection at
end of treatment
Secondary
Inhibition of disease progression
Reduction of incidence of hepatocellular
carcinoma
Reduction in need for liver transplant

81
Treatment Definitions

The First aim is to clear HCV RNA from peripheral
blood, a necessary, but not sufficient condition
to achieve a sustained virological response.

The Second aim is to prevent relapse in patients
who cleared HCV RNA during induction, in order to
achieve a sustained virological response

Adapted from Pawlotsky JM, Hepatology vol. 32,
5, 2000
82
Patterns of Response to InitialAntiviral Therapy
83
Changing Paradigms

Speed of response is an important predictor of
sustained virologic response.
66 of patients with HCV genotypes 2 and 3 had
undetectable HCV levels within 4 weeks of
treatment
Sustained virologic response.
90 for 24 week treatment arm
75 for 16 week treatment
Relapse rates
18 for 24 week treatment
31 for 16 week treatment

Shiffman, et al., N. Eng. J. Med 2007357124-134
84
Resources

S.C. Hepatitis C Coalition
SC DHEC Hepatitis Nurse Consultant
Elona Rhame, RN
Pharmaceutical Companies
Physician Referral List

85
SC Hepatitis C Coalition

803-898-9562

Mick Carnett, CDP, CRPS, D.Div., Executive
Director
Informational support services to providers
patients
Brochures/literature
Presentations
Annual Statewide Hepatitis C Summit
Statewide Physicians Referral List
ETV program, HCC videos, PSAs

86
Surveillance/Reporting

Hepatitis C is reportable to the health
department within 7 days.
Acute and chronic HCV cases are reported by
health department to CDC via CHESS.

87
Hepatitis B
88
Clinical Features

Incubation period Mean 60-90 days
Range 45-180 days
Clinical illness (jaundice) lt5 yrs, lt10
?5 yrs, 30-50
Acute case-fatality rate 0.5-1
Chronic infection lt5 yrs, 30-90 ?
5 yrs, 2-10
Premature mortality fromchronic liver disease
15-25

89
Geographic Distribution of Chronic HBV Infection
HBsAg Prevalence
?8 - High
2-7 - Intermediate
lt2 - Low
Source Centers for Disease Control and
Prevention
90
Hepatitis B Surface Antigen

HBsAg
Detection of acutely or chronically infected
individuals. Antigen components used in HBV
vaccine
Should undergo testing to assess the status of
their liver disease
Assess hepatic synthetic function serum albumin,
prothrombin time
Assess for hypersplenism CBC (plts, wbc
decreased)
Assess for viral replication status HBeAg and
HBV DNA

91
Antibody to HBsAg

Anti-HBsAg
Identification of individuals who have resolved
HBV infections.
Determination of immunity after immunization.

92
Hepatitis B Envelope Antigen

HBeAg
Identification of infected individuals at
increased risk for transmitting HBV

93
Antibody to HBe

HBeAb or anti-HBe
Identification of infected individuals with lower
risk for transmitting HBV

94
Antibody to HBV Core Antigens

Anti-HBc or HBcAb
Identification of persons with acute, resolved,
or chronic HBV infection.
Anti-HBc is not present after immunization.

95
IgM Antibody to HBcAg

IgM anti-HBc or HBc IgM
Identification of acute or recent HBV infections
(including those in HBsAg-negative persons during
the window phase of infection)

96
Acute HBV Infection with Recovery
Symptoms
anti-HBe
HBeAg
Total anti-HBc
Titer
anti-HBs
IgM anti-HBc
HBsAg
0
4
8
12
16
20
24
28
32
36
52
100
Weeks after Exposure
97
Progression to Chronic HBV Infection
Acute (6 months)
Chronic (Years)
HBeAg
anti-HBe
HBsAg
Total anti-HBc
Titer
IgM anti-HBc
Years
0
4
8
12
16
20
24
28
32
36
52
Weeks after Exposure
98
Chronic Hepatitis B Infection

Defined as testing positive for the HBsAg for
more than 6 months
Patients are at increased risk for progressive
liver disease and hepatocellular carcinoma

99
35 year old Medical Technologist who cut her
hand. She was removing the top from a Vacutainer
tube when the tube broke.

Test Result
HBsAg Negative
Anti-HBc Negative
Anti-HBc-IgM Negative
Anti-HBs Positive
Anti-HBs Ratio 23.1

100
29 year old automotive engineer who
presented with fatigue x 2 weeks and mild
jaundice. Liver enzyme levels were significantly
elevated.

Test Result
HBsAg Positive
Anti-HBc Positive
Anti-HBc-IgM Positive
Anti-HBs Negative
Anti-HBs Ratio lt2.1

101
James is a 23 year old food service employee. He
was tested as part of his pre-employment physical
examination. He was diagnosed with HBV infection
one year ago.

HBsAg Positive
Anti-HBc Positive
Anti-HBc-IgM Negative
Anti-HBs Negative
HBe Ag Positive
Anti-Hbe Negative

What is his HBV Status?
102
Chronic Active Hepatitis

High levels of HBV in blood
Increased risk of cirrhosis
Increased risk of liver cancer

103
James, a 23 year old food service employee. He
was tested as part of his pre-employment physical
examination. He was diagnosed with HBV infection
one year ago.

High viral load
Increased risk of virus transmission

Can he work as a food handler in your hospital?
104
HBV Transmission

Parenteral
Sexual
Perinatal
Risk of transmission increases with the level of
HBV DNA in serum and HBeAg positive

105
HBV Concentrations in Various Body Fluids
Low/Not
High
Moderate
Detectable
blood
semen
urine
serum
vaginal fluid
feces
wound exudates
saliva
sweat
tears
breast milk
106
Outcome of HBV Infection
107
Chronic HBV Infection

Immune tolerant patient
HBeAg positive and HBeAb negative
Viral load 100,000 to 1 billion copies/mL
Normal ALT
No necroinflammation in the liver
Chronic Active Hepatitis B (Viral Load gt 100,000
cy/mL)
HBeAg positive (wild type virus)
HBeAg negative (pre core or core promoter
mutants)
Elevated ALT and/or active liver biopsy
Increased risk for progression to cirrhosis and
ESL disease and candidates for therapy

108
Chronic HBV Infection

Inactive HBsAg Carrier
HBeAg negative and HBeAb positive
Viral load 100 to 10,000 copies/mL
Normal ALT
Resolution of necroinflammation in the liver
Reduced risk of progressive liver disease
Resolution
HBsAg negative, HBsAb positive
Viral load ltltlt 20,000 copies/mL
HBeAg negative and HBeAb positive
Normal ALT

109
HBV DNA Testing

Assess of viral replication in chronic HBsAg
carriers.
Assess the risk of progression toward cirrhosis
and hepatocellular carcinoma.
Decision to treat.
Assess treatment efficacy and failure

110
Hepatitis B Vaccine

Licensed in 1982 currently recombinant (in US)
3 dose series, typical schedule 0, 1-2, 4-6
months - no maximum time between doses (no need
to repeat missed doses or restart)
2 dose series (adult dose) licensed by FDA for
11-15 year olds (Merck)
Protection 30-50 dose 1 75 - 2 96 - 3
lower in older, immunosuppressive illnesses
(e.g., HIV, chronic liver diseases, diabetes),
obese, smokers

111
Indications for Pre-Exposure Vaccination

Children lt 19 yrs of age
Persons at risk for sexual transmission.
MSM
Current/past IDU
Family member of HBsAg adoptees
Persons at occupational risk
Hemodialysis patients

112
Indications for Pre-Exposure Vaccination

Clients/staff of institutions for developmentally
disabled
Persons receiving clotting factors
International travelers in high/intermediate
areas
Inmates
Adults 19 years of age older desiring protection

113
Indications for Post-Exposure Prophylaxis

Infants born to HBsAg mothers
Persons who have percutaneous or permucosal
exposure to blood
Sex partners of persons with acute HBV
Household contacts of persons with acute HBV if
blood exposure or if unimmunized infant
Sex partners of persons with chronic HBV
Household contacts of persons with chronic HBV
Victims of sexual assault

114
Indications for Pre-Vaccination Serologic
Testing

Unimmunized sexual contacts of persons with acute
and chronic Hepatitis.
Unimmunized household contacts of persons with
acute HBV if there has been a blood exposure.
Unimmunized household contacts of person with
chronic HBV.
Unimmunized persons in populations with high
rates of HBV (IDU, inmates)

115
Indications for Post-Vaccination Serologic
Testing

Persons at occupational risk
Infants born to HBsAg mothers
Immunocompromised persons

116
Sexual Contacts to Acute HBV

Sexual contacts of persons with acute HBV
regardless of age
Test if unimmunized
Administer HBIG and first hep B dose at time test
is obtained.
If negative, continue hepatitis vaccination
series.

117
Household Contacts to Acute Cases

Children (gt12 months of age), Adolescents, and
Adult Household Contacts to Acute Cases
Not at increased risk unless blood exposure.
Only if blood exposure has occurred in past 14
days, test and give HBIG and first dose of
hepatitis B vaccine.
If negative, continue vaccination series.

118
Sexual and Household Contacts to Chronic Cases

Sexual Contacts (regardless of age)
If unimmunized, test and give first dose of
vaccine.
If test is negative, continue series.
Household Contacts (regardless of age)
If unimmunized, test and give first dose of
vaccine.
If test is negative, continue series.

119
Victims of Sexual Assault

If offender is HBsAg positive or status is
unknown and victim is unimmunized
If offender has acute HBV infection - give HBIG
and hepatitis B vaccine.
If offender has chronic HBV infection give
vaccine.

120
Healthcare Worker Pre-Exposure Vaccination

Administer vaccination series.
Obtain postvaccination serology at 1-2 months
after completion of series.
If anti-HBs levels are gt 10 mIU/mL, employee is a
responder.
If anti-HBs levels are lt 10 mIU/mL, employee is a
non-responder. Revaccinate and repeat serology.

121
Postvaccination Serology Testing-

Infants born to HBsAg positive mothers.
Persons at high risk of occupational exposure.
Persons who are immunocompromised and at
continued risk of infection.
Persons receiving clotting factors.

122
Postvaccination Testing

Persons who were tested 1-2 months after
completion of series and had anti-HBs levels gt 10
mIU/mL should not receive any further testing.

123
Approved Therapies for HBV Infection

Interferons
Interferon alpha 2b (5 million units qd or 10
million units TIW for 12-24 weeks)
Pegylated interferon alpha 2a (180 ug once/week
for 48 weeks)
Nucleoside analogues
Lamivudine (100 mg qd)
Entecavir (0.5 mg qd 1 mg if lamivudine
resistance)
Nucleotide analogues
Adefovir (10 mg qd)

124
Hepatitis B Surveillance

Acute Hepatitis B is an urgently reportable
condition. It must be reported by phone to the
health department within 24 hours.
Chronic Hepatitis B is a reportable condition and
must be reported to health department within 7
days.
Perinatal Hepatitis B is a reportable condition
and must be reported to health department within
7 days.

125
Hepatitis D Virus
126
HDV Transmission

Percutanous exposures
injecting drug use
Permucosal exposures
sex contact

127
Geographic Distribution of HDV Infection
Taiwan
Pacific Islands
HDV Prevalence
High
Intermediate
Low
Very Low
No Data
Source Centers for Disease Control and Prevention
128
Hepatitis D - Clinical Features

Coinfection
severe acute disease
low risk of chronic infection
Superinfection
usually develop chronic HDV infection
high risk of severe chronic liver disease

129
HBV - HDV Coinfection
Symptoms
ALT Elevated
anti-HBs
Titer
IgM anti-HDV
HDV RNA
HBsAg
Total anti-HDV
Time after Exposure
130
HBV - HDV Superinfection
Jaundice
Symptoms
Total anti-HDV
ALT
Titer
HDV RNA
HBsAg
IgM anti-HDV
Time after Exposure

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