Key Facts: Geographical Distribution

Download as odt, pdf, or txt
Download as odt, pdf, or txt
You are on page 1of 4

Hepatitis B is a potentially life-

Key facts threatening liver infection caused by


the hepatitis B virus (HBV). It is a
• Hepatitis B is a viral infection that attacks the liver and
major global health problem. It can
can cause both acute and chronic disease. cause chronic infection and puts
• The virus is most commonly transmitted from motherpeople to at high risk of death from
child during birth and delivery, as well as through contact
cirrhosis and liver cancer.
with blood or other body fluids.
• WHO estimates that in 2015, 257 million people wereA safe and effective vaccine that offers a
living with chronic hepatitis B infection (defined as 98-100% protection against hepatitis B is
hepatitis B surface antigen positive). available. Preventing hepatitis B infection
• In 2015, hepatitis B resulted in an estimated 887 000 averts the development of complications
deaths, mostly from cirrhosis and hepatocellular including the development of chronic
carcinoma (i.e. primary liver cancer). disease and liver cancer.

• As of 2016, 27 million people (10.5% of all people


estimated to be living with hepatitis B) were aware ofGeographical distribution
their infection, while 4.5 million (16.7%) of the people
Hepatitis B prevalence is highest in the
diagnosed were on treatment.
WHO Western Pacific Region and the
• Hepatitis B can be prevented by vaccines that are safe, WHO African Region, where 6.2% and
available and effective. 6.1% of the adult population is infected
respectively. In the WHO Eastern
Mediterranean Region, the WHO South-
East Asia Region and the WHO European Region, an estimated 3.3%, 2.0% and 1.6% of the general population is
infected, respectively. And in the WHO Region of the Americas, 0.7% of the population is infected.

Transmission
In highly endemic areas, hepatitis B is most commonly spread from mother to child at birth (perinatal transmission),
or through horizontal transmission (exposure to infected blood), especially from an infected child to an uninfected
child during the first 5 years of life. The development of chronic infection is very common in infants infected from their
mothers or before the age of 5 years.

Hepatitis B is also spread by needlestick injury, tattooing, piercing and exposure to infected blood and body fluids,
such as saliva and, menstrual, vaginal, and seminal fluids. Sexual transmission of hepatitis B may occur, particularly
in unvaccinated men who have sex with men and heterosexual persons with multiple sex partners or contact with sex
workers.
Infection in adulthood leads to chronic hepatitis in less than 5% of cases, whereas infection in infancy and early
childhood leads to chronic hepatitis in about 95% of cases. Transmission of the virus may also occur through the
reuse of needles and syringes either in health-care settings or among persons who inject drugs. In addition, infection
can occur during medical, surgical and dental procedures, through tattooing, or through the use of razors and similar
objects that are contaminated with infected blood.

The hepatitis B virus can survive outside the body for at least 7 days. During this time, the virus can still cause
infection if it enters the body of a person who is not protected by the vaccine. The incubation period of the hepatitis B
virus is 75 days on average, but can vary from 30 to 180 days. The virus may be detected within 30 to 60 days after
infection and can persist and develop into chronic hepatitis B.
Symptoms
Most people do not experience any symptoms when newly infected. However, some people have acute illness with
symptoms that last several weeks, including yellowing of the skin and eyes (jaundice), dark urine, extreme fatigue,
nausea, vomiting and abdominal pain. A small subset of persons with acute hepatitis can develop acute liver failure,
which can lead to death.

In some people, the hepatitis B virus can also cause a chronic liver infection that can later develop into cirrhosis (a
scarring of the liver) or liver cancer.

Who is at risk of chronic disease?


The likelihood that infection becomes chronic depends on the age at which a person becomes infected. Children less
than 6 years of age who become infected with the hepatitis B virus are the most likely to develop chronic infections.

In infants and children:

• 80–90% of infants infected during the first year of life develop chronic infections; and
• 30–50% of children infected before the age of 6 years develop chronic infections.
In adults:
• less than 5% of otherwise healthy persons who are infected as adults will develop chronic
infections; and
• 20–30% of adults who are chronically infected will develop cirrhosis and/or liver cancer.

HBV-HIV coinfection
About 1% of persons living with HBV infection (2.7 million people) are also infected with HIV. Conversely, the global
prevalence of HBV infection in HIV-infected persons is 7.4%. Since 2015, WHO has recommended treatment for
everyone diagnosed with HIV infection, regardless of the stage of disease. Tenofovir, which is included in the
treatment combinations recommended as first-line therapy for HIV infection, is also active against HBV.

Diagnosis
It is not possible, on clinical grounds, to differentiate hepatitis B from hepatitis caused by other viral agents, hence,
laboratory confirmation of the diagnosis is essential. A number of blood tests are available to diagnose and monitor
people with hepatitis B. They can be used to distinguish acute and chronic infections.

Laboratory diagnosis of hepatitis B infection focuses on the detection of the hepatitis B surface antigen HBsAg. WHO
recommends that all blood donations be tested for hepatitis B to ensure blood safety and avoid accidental
transmission to people who receive blood products.

• Acute HBV infection is characterized by the presence of HBsAg and immunoglobulin M (IgM)
antibody to the core antigen, HBcAg. During the initial phase of infection, patients are also
seropositive for hepatitis B e antigen (HBeAg). HBeAg is usually a marker of high levels of
replication of the virus. The presence of HBeAg indicates that the blood and body fluids of the
infected individual are highly infectious.
• Chronic infection is characterized by the persistence of HBsAg for at least 6 months (with or
without concurrent HBeAg). Persistence of HBsAg is the principal marker of risk for
developing chronic liver disease and liver cancer (hepatocellular carcinoma) later in life.
Treatment
There is no specific treatment for acute hepatitis B. Therefore, care is aimed at maintaining comfort and adequate
nutritional balance, including replacement of fluids lost from vomiting and diarrhoea. Most important is the avoidance
of unnecessary medications. Acetaminophen/Paracetamol and medication against vomiting should not be given.

Chronic hepatitis B infection can be treated with medicines, including oral antiviral agents. Treatment can slow the
progression of cirrhosis, reduce incidence of liver cancer and improve long term survival. Only a proportion
(estimates vary from 10% to 40% depending on setting and eligibility criteria) of people with chronic hepatitis B
infection will require treatment.

WHO recommends the use of oral treatments - tenofovir or entecavir- as the most potent drugs to suppress hepatitis
B virus. They rarely lead to drug resistance compared with other drugs, are simple to take (1 pill a day), and have few
side effects, so require only limited monitoring.

Entecavir is off-patent. In 2017, all low- and middle-income countries could legally procure generic entecavir, but the
costs and availability varied widely. Tenofovir is no longer protected by a patent anywhere in the world. The median
price of WHO-prequalified generic tenofovir on the international market fell from US$ 208 per year to US$ 32 per year
in 2016.

In most people, however, the treatment does not cure hepatitis B infection, but only suppresses the replication of the
virus. Therefore, most people who start hepatitis B treatment must continue it for life.

There is still limited access to diagnosis and treatment of hepatitis B in many resource-constrained settings. In 2016,
of the 257 million people living with HBV infection, 10.5% (27 million) were aware of their infection. Of those
diagnosed, the global treatment coverage is 16.7% (4.5 million). Many people are diagnosed only when they already
have advanced liver disease.

Among the long-term complications of HBV infections, cirrhosis and hepatocellular carcinoma cause a large disease
burden. Liver cancer progresses rapidly, and since treatment options are limited, the outcome is generally poor. In
low-income settings, most people with liver cancer die within months of diagnosis. In high-income countries, surgery
and chemotherapy can prolong life for up to a few years. Liver transplantation is sometimes used in people with
cirrhosis in high income countries, with varying success.

Prevention
The hepatitis B vaccine is the mainstay of hepatitis B prevention. WHO recommends that all infants receive the
hepatitis B vaccine as soon as possible after birth, preferably within 24 hours. Routine infant immunization against
hepatitis B has increased globally with an estimated coverage (third dose) of 84% in 2017. The low prevalence of
chronic HBV infection in children under 5 years of age, estimated at 1.3% in 2015, can be attributed to the
widespread use of hepatitis B vaccine. In most cases, 1 of the following 2 options is considered appropriate:
• a 3-dose schedule of hepatitis B vaccine, with the first dose (monovalent) given at birth and the
second and third doses (monovalent or combined vaccine) given at the same time as the first
and third doses of diphtheria, pertussis (whooping cough), and tetanus – (DTP vaccine); or
• a 4-dose schedule, where a monovalent birth dose is followed by 3 monovalent or combined
vaccine doses, usually given with other routine infant vaccines.
The complete vaccine series induces protective antibody levels in more than 95% of infants, children and young
adults. Protection lasts at least 20 years and is probably lifelong. Thus, WHO does not recommend booster
vaccinations for persons who have completed the 3 dose vaccination schedule.
All children and adolescents younger than 18 years and not previously vaccinated should receive the vaccine if they
live in countries where there is low or intermediate endemicity. In those settings it is possible that more people in
high-risk groups may acquire the infection and they should also be vaccinated. This includes:

• people who frequently require blood or blood products, dialysis patients and recipients of solid
organ transplantations;
• people in prisons;
• people who inject drugs;
• household and sexual contacts of people with chronic HBV infection;
• people with multiple sexual partners;
• healthcare workers and others who may be exposed to blood and blood products through their
work; and
• travellers who have not completed their HBV series, who should be offered the vaccine before
leaving for endemic areas.

You might also like