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HEPATITIS B

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Title: HEPATITIS B

1
HEPATITIS B

Anna S. F. Lok, MD
University of Michigan
Ann Arbor, MI

2
What is Hepatitis B?

Hepatitis B is an infection of the liver caused
by the hepatitis B virus

3
How common is hepatitis B?

Worldwide
400 million people are chronic carriers
About 75 of HBV carriers live in Asia
0.5-1 million deaths per year due to HBV
Asia
Liver cancer is the 2nd cancer killer among Asian
men and the 5th cancer killer among Asian women
Roughly 40 of Asian men and 15 of Asian women
with chronic hepatitis B die of a liver-related
illness

4
Geographic Distribution of Chronic HBV Infection
HBsAg Prevalence
?8 - High
2-7 - Intermediate
lt2 - Low
5
Hepatitis B and Asian Americans

Less than 0.5 (1 in 200) Americans have chronic
hepatitis B
About 10-15 (1 in 8 to 10) Asian Americans have
chronic hepatitis B
About 50 (1 in 2) of the people in the US with
chronic hepatitis B are Asian Americans
A much higher percent of Asian Americans compared
to Americans of other races have hepatitis B

6
Why is Hepatitis B so common among Asian
Americans?

Hepatitis B is very common in Asia
Many Asian Americans were infected with hepatitis
B before they came to the US
Asian Americans born in the US may be infected
through their mother or other family members, who
are HBV carriers

7
Hepatitis B and Asian Americans

National Health and Nutrition Examination Survey
(NHANES)
Survey on prevalence of various diseases in the
US
Sampled cohorts representative of US population
African Americans and Hispanics over sampled to
ensure sufficient number studied to permit
conclusions on prevalence of diseases among those
racial/ethnic groups
Reliable data not available for Asian Americans
because Asians not over sampled, number studied
too small to be conclusive, and Asians lumped as
other racial/ethnic groups

8
Hepatitis B and Asian Americans

NHANES III 1988-1994
Current and past HBV infection 4.9
Chronic HBV infection 0.4
Highest prevalence among blacks
5-15 among immigrants from Central and
Southeast Asia, Middle East and Africa
Prevalence data for Asians not available

9
Why is it that hepatitis B gets so little
attention in the US?

Federal and state governments public health
Overall prevalence is low not a very common
problem here
Most of those affected by HBV are Asians who
are politically silent (squeaky wheel gets the
oil)
NIH, CDC, Scientific organizations research and
education
Not a common problem
With an effective vaccine, hepatitis B will be
eradicated in the next generation.. we predicted
that in the 1980s
Competition for and attention from other more
trendy diseases HIV, HCV, SARS, avian flu,
cancers.

10
How is HBV spread?

HBV is more easily spread than HIV (virus that
causes AIDS) and HCV
HBV can live outside the human body for up to 7
days
People with chronic hepatitis B can have very
large amounts of virus in their blood serum HBV
DNA up to 11 log10 copies/mL (100 billion)

11
How is HBV spread?

Mainly through blood and bodily secretions
Infected mother to babies at birth
Contact with blood from carriers through wounds,
contaminated household articles such as razors,
toothbrushes, or contaminated needles used for
tattoos and injecting drugs
Sexual contact with carriers

12
How is HBV spread?

HBV is not spread by
Hugging or kissing
Coughing or sneezing
Sharing eating utensils

13
Outcome of Acute HBV Infection
Recovery
Acute Hepatitis
SubclinicalHepatitis
FulminantHepatitis
Death
Acute Infection
Chronic Infection
14
What is Hepatitis B?

Hepatitis B may be ACUTE
Recent infection
May have no symptoms, especially in children
Common symptoms easily tired, poor appetite,
nausea, abdominal discomfort, jaundice
Roughly 95 recover, usually in 2-3 months
About 1 severe hepatitis with acute liver
failure
About 5 go on to chronic infection, lasts longer
than 6 months

15
Risk of Chronic HBV Infection
16
Outcome of Chronic HBV Infection
Chronic HBV Infection
Inactive Carrier State
Chronic Hepatitis
Cirrhosis
HCC
17
What is Hepatitis B?

Hepatitis B may be CHRONIC
Long-lasting infection, persists for more than 6
months
Most people have no symptoms
Common symptoms easily tired, poor appetite,
nausea, abdominal discomfort
Can go on to cirrhosis, liver failure, liver
cancer, and death

18
How can hepatitis B be diagnosed?

The only way to know is to have a blood test
Most people with hepatitis B have no symptoms
until late stages of liver disease
Tests for hepatitis B or liver enzymes are not
included in most routine check-ups
Hepatitis B may be present even if liver enzymes
were tested and were normal

19
Serological Markers of HBV Infection?????????????
?????

HBsAg Acute/Chronic infection
Anti-HBc IgM Recent infection
HBeAg High infectivity
Anti-HBe Low infectivity
Anti-HBs Immunity
Anti-HBc IgG HBsAg Chronic infection
Anti-HBc IgG anti-HBs Resolved infection

20
Acute HBV Infection
HBV DNA
HBeAg
Anti-HBe
Anti-HBe
Anti-HBs
Anti-HBc
HBsAg
Anti-HBc IgM
0 2
4 6

Months
Years
21
Chronic HBV Infection
22
Serum HBV DNA is the most reliable marker of HBV
replication and infectivity

Fluctuating levels, serial tests important for
clinical assessment
Virus persists at low levels even after recovery
Reactivation can occur spontaneously and more
often when immune system is suppressed
HBV DNA levels do not always correlate with ALT
levels or histologic activity of liver disease
Persistently high serum HBV DNA levels are
associated with increased risk of cirrhosis and
HCC

23
Hepatitis B Vaccines

Genetically engineered hepatitis B surface
antigen only
3 doses month 0, 1, 6
Immune response 50 after 1 dose
95 after 3 doses
Duration of protection gt15 years, dependent on
initial antibody response
Factors associated with poor response older age,
chronic medical illness (cirrhosis, kidney
failure, diabetes), decreased immune response,
smoking, obesity, genetics

24
Indications for HBV Vaccines

Hepatitis B immune globulin and HB vaccine to
infants of HBsAg mothers
All infants
All children and adolescents who were not
vaccinated at birth
Vaccination of adults at risk of infection
Occupational
Sexual / household contacts
Injection drug users
Long-term residence in high prevalence areas

25
HBV Vaccine Safety

Worldwide, more than 500 million individuals
have received HB vaccine over the past 20 years
Most common adverse event soreness and
erythema at the injection site
Systemic symptoms transient low-grade
fever, headache, malaise and myalgia in 10

26
Impact of HBV vaccination on HBV infection rates
in Taiwanese children
30
HBsAg
Anti-HBc
20

10
0
?
1984
1994
1999
Vaccination of infants born to HBsAg mother
Universal vaccination of infant/preschool children
Ni YH, Ann Intern Med 2001135796
27
Impact of HBV Vaccination on Incidence of HCC
in Taiwanese Children
?
Universal Vaccination of Newborns
Chang MH, NEJM 19973361855
28
Hepatitis BFactors affecting disease activity
and progression
VIRUS Genotype Molecular Variants
HOST Gender Age Immune Response Genetics
ENVIRONMENT Alcohol HCV, HDV, HIV Carcinogens
29
Stages of chronic HBV infection
Immune
Immune
Low replicative
Reactivation
tolerance
clearance
phase
phase
HBeAg - / anti-HBe (PC/CP variants)
HBeAg (wild)
lt
lt
gt
gt
gt105 cp/ml
HBV-DNA
lt105 cp/ml
109-1010 cp/ml
107-108 cp/ml
ALT
Normal / mild CH
moderate/severe CH
moderate/severe CH
Normal/mild CH
cirrhosis
cirrhosis
Inactive cirrhosis
Inactive-carrier state
HBeAg Chronic hepatitis
HBeAg Chronic hepatitis
30
Unique Aspects of Hepatitis B among Asians

Clinical Manifestations/Natural history
Immune tolerant phase
Frequent exacerbations and reactivations
Increased risks of HCC

31
Immune Tolerant Phase

First 10-30 years of perinatally acquired HBV
infection
Asymptomatic
High HBV DNA levels but normal ALT
Very low rates of spontaneous/treatment-induced
HBeAg seroconversion

32
Immune Clearance Phase
HBeAg ? anti-HBe seroconversion Predictors
ALT, age, gender, HBV genotype Annual rate
5-15 Hepatitis Flares ? HBeAg seroconversion
preceded by flares ¼ flares followed by HBeAg
seroconversion More common in men Increased
risk of cirrhosis
33
Stages of chronic HBV infection
Immune
Immune
Low replicative
Reactivation
tolerance
clearance
phase
phase
HBeAg - / anti-HBe (PC/CP variants)
HBeAg (wild)
lt
lt
gt
gt
gt105 cp/ml
HBV-DNA
lt105 cp/ml
109-1010 cp/ml
107-108 cp/ml
ALT
Normal / mild CH
moderate/severe CH
moderate/severe CH
Normal/mild CH
cirrhosis
cirrhosis
Inactive cirrhosis
Inactive-carrier state
HBeAg Chronic hepatitis
HBeAg Chronic hepatitis
34
Inactive HBsAg Carrier State

HBsAg gt 6 months
HBeAg- , anti-HBe
Serum HBV DNA lt 103 copies/ml
Persistently normal ALT
Outcome dependent on liver damage accrued prior
to entering inactive carrier state and any
subsequent reactivation

35
HBeAg Chronic Hepatitis B

HBsAg
HBeAg
Serum HBV DNA gt 104-5 copies/ml
Elevated ALT / moderate-severe inflammation
on biopsy
Frequently associated with precore or core
promoter mutations that prevent or decrease
HBeAg production

36
Risk factors for progression to cirrhosis
Viral factors Host Factors
External Factors

Persistently high HBV DNA levels
HBV precore/CP variant?
HBV genotype (C gt B)

Older age
Male gender
Advanced fibrosis
Persistent ALT elevation
Recurrent hepatitis flares
HDV, HCV coinfections
HIV coinfection

Alcohol

37
Risk factors for progression to HCC
Viral factors Host Factors
External Factors

Persistently high HBV DNA levels
HBV CP variant
HBV genotype (C gt B)

Older age
Male gender
Asians??
Advanced fibrosis
Persistent ALT elevation
Recurrent hepatitis flares
HDV, HCV coinfections
HIV coinfection
Family history of HCC

Alcohol
Aflatoxin
Smoking

38
What can patients do to protect their liver?

Do not drink alcohol
Do not take any herbal medicine that might hurt
the liver
Eat a balanced diet, exercise regularly, avoid
getting overweight
Hepatitis B is a chronic health problem, HBV
levels and severity of liver damage can change
with time, see their doctor and get tested at
least once a year even if they have no symptoms

39
Treatment of Chronic Hepatitis B

Goals
Suppression of HBV replication
Decrease hepatic necroinflammation and fibrosis
Prevent progression to cirrhosis, liver failure
and HCC

40
Treatment of Chronic Hepatitis BDefinition of
Response

HBeAg patients
Serum HBV DNA decrease to lt100,000 copies/ml
Loss of HBeAg anti-HBe seroconversion
Normalization of ALT level
HBeAg- patients
Serum HBV DNA decrease to undetectable by PCR
Normalization of ALT level
On-treatment response initial / maintained
Off-treatment sustained response FU mo 6 or 12

Lok A et al., Gastro 20011201828
41
Randomized controlled trial of lamivudine in
patients with advanced liver disease HBeAg
and/or serum HBV DNA gt700,000 gEq/mL
with disease progression
21
Placebo
P0.001
9
Lamivudine
Time to disease progression (months)
Placebo (n215) ITT
population Lamivudine
(n436) p0.001
Liaw YF, NEJM 2004 3511521
42
Licensed HBV therapies and those under
development

43
Who Should be Treated?

Not a question of who to treat but when treat
now or monitor and treat when indicated
All HBV carriers are potential treatment
candidates
A patient who is not a treatment candidate now
can be a treatment candidate in the future
Changes in HBV replication status and/or
activity/stage of liver disease
Availability of new and better treatments

44
When to start treatment?
Benefits
Risks
Likelihood of sustained response cirrhosis
and HCC
Side effects Drug resistance
Patients age Co-morbid illness Costs
Likelihood of cirrhosis / HCC in the next 10-20
yrs Likelihood of sustained viral suppression
after a defined course of treatment
45
What should be the primary treatment?
Long-term Benefits
Long-term Risks
Antiviral potency Durability of response
Side effects Drug resistance
Contraindications Ease of administration Duration
of Rx Costs of Rx monitoring Patient and
provider preference
46

47
When can treatment be stopped?