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Originally known
as serum hepatitis, Hepatitis B has only been
recognized as such since World War II, and has
caused current epidemics in parts of Asia and
Africa. Hepatitis B is recognized as endemic in
China and various other parts of Asia.
Over
one-third of the world's population has been or is
actively infected by hepatitis B.
Hepatitis B is
largely transmitted through exposure to bodily
fluids containing the virus. This includes
unprotected sexual contact, blood transfusions,
re-use of contaminated needles and syringes,
vertical transmission from mother to child during
childbirth, and so on. The primary method of
transmission depends on the prevalence of the
disease in a given area. In
low prevalence areas, such as the continental United
States, IV drug abuse and unprotected sex are the
primary method.
In moderate prevalence areas, Hepatitis B is
predominantly spread among children. In high
prevalence countries, such as China, vertical
transmission is most common.
Without intervention, a mother who is positive for
the Hepatitis B surface
antigen confers a 20% risk of passing the infection
to her offspring at the time of birth. This risk is
as high as 90% if the mother is also positive for
the Hepatitis B e antigen.
Roughly 16-40% of
unimmunized sexual partners of individuals with
hepatitis B will be infected through sexual contact.
The virus that
causes hepatitis B is a member of the Hepadnavirus
family and it is composed of an icosahedral
nucleocapsid (core) enclosing a circular,
double-stranded DNA genome. The virus is unique
amongst the DNA viruses in that it uses a reverse
transcriptase to generate the genomic DNA to deliver
to its progeny. Additionally, the DNA genome is
incomplete on one strand. Hepatitis D infection
requires a concomitant infection with hepatitis B.
Co-infection with Hepatitis D increases the risk of
liver cirrhosis and subsequently,
liver cancer.
Hepatitis B Symptoms
Symptoms of
Hepatitis B infection may lead to
a chronic
inflammation of the liver, leading to cirrhosis. In
looking at the long term affects of Hep B, this type
of infection dramatically increases the incidence of
liver cancer.
The greater a
person's age at the time of infection, the greater
the chance their body will clear the infection.
More
than 95% of people who become infected as adults or
older children will stage a full recovery and
develop
protective immunity to the virus.
However, only 5% of neonates that acquire the
infection from their mother at birth will clear the
infection. Seventy percent of those infected between
the age of one to six will clear the infection. When
the infection is not cleared, one becomes a chronic
carrier of the virus.
Hepatitis B Treatment
There are
currently several treatments for chronic hepatitis B
that can increase a person's chance of clearing the
infection. Treatments are available in the form of
antivirals such as lamivudine and adefovir and
immune system modulators such as interferon alpha.
There are several other antivirals under
investigation. Roughly, all of the currently
available treatments, when used alone, are about
equally efficacious. However, some individuals are
much more likely to respond than others. It is not
presently known if combination therapy offers any
advantages. In general, each works by reducing the
viral load by several orders of magnitude thus
helping a body's immune system clear the infection.
Treatment strategies should be individualized by a
doctor and patient. Considerations include the risks
associated with each treatment, a person's
likelihood of clearing the virus with treatment, a
person's risk for developing complications of
persistent infection, and development of viral
resistance with treatment.
Transfer
Factor is nature's most powerful
immune modulators
Chronic carriers
should be strongly encouraged to avoid consuming
alcohol as it increases their risk for cirrhosis and
hepatocellular carcinoma (liver cancer).
Infants born to
mothers known to carry Hepatitis B can be treated
with antibodies to the hepatitis B virus (Hepatitis
B immune globulin or HBIG). When given with the
vaccine within twelve hours of birth, the risk of
acquiring Hepatitis B is reduced 95%. This treatment
also allows a mother to safely breastfeed her child.
An individual
exposed to the virus that has never been vaccinated
may also be treated with HBIG (Hepatitis
B immune globulin) just after the
exposure. For instance, a health care worker
accidentally stuck by a needle used in a hepatitis B
carrier would qualify. Treatment must be soon after
exposure, however.
Molecular Biology of Hepatitis B
A recombinant
vaccine is available to prevent hepatitis B. Many
countries now routinely vaccinate infants against
hepatitis B. In many areas, vaccination against
hepatitis B is also required for all healthcare
workers. Booster doses are recommended every five to
ten years for healthcare workers.
Prevention of
Hepatitis B
The Hepatitis B
virus particle consists of a proteinaceous core
particle containing the viral genome in DNA form and
an outer lipid-based envelope with embedded
proteins. The envelope proteins are involved in
viral binding and release into susceptible cells.
The inner capsid relocates the DNA genome to the
cell's nucleus where viral mRNAs are transcribed.
Three subgenomic transcripts encoding the envelope
proteins are made, along with a poorly understood
transcript encoding the X protein, whose function is
still under debate. A fourth pre-genomic RNA is
transcribed, which is exported to the cytosol and
translates the viral polymerase and core proteins.
Polymerase and pre-genomic RNA are encapsidated in
assembling core particles, where reverse
transcription of the pre-genomic RNA to genomic DNA
occurs by the polymerase protein. The mature core
particle then exits the cell via normal secretory
pathways, acquiring an envelope along the way.
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