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Kinds of Ebola
The virus takes its name from the Ebola River in the
northern Congo basin of central Africa, where it first emerged in 1976. Ebola
is closely related to the Marburg virus,
which was discovered in 1967, and the two are the only members of the
Filoviridae that cause epidemic human disease. Five strains of Ebola virus,
known as Ebola-Zaire, Ebola-Sudan,
Ebola-Côte d'Ivoire, Ebola-Reston,
and Ebola-Bundibugyo, named for their outbreak
locations, have been described.
Ebola-Zaire causes death in 80 to 90 percent of cases,
and Ebola-Sudan causes death in 50 percent of cases. Ebola-Côte d'Ivoire, found
in dead chimpanzees in the Taï National Park in southwestern Côte d'Ivoire, can
infect humans, although only two human cases have been documented, and both
individuals survived. Ebola-Reston, which was originally discovered in
laboratory monkeys in Reston, Va., in 1989, was also detected in laboratory
monkeys in other locations in the United States in 1990 and 1996, as well as in
Siena, Italy, in 1992. All the monkeys infected with Ebola-Reston have been
traced to one export facility located in the Philippines, although the origin
of the strain has not been identified. Similar to Ebola-Côte d'Ivoire,
Ebola-Reston does not appear to cause death in humans. The fifth strain,
Ebola-Bundibugyo, was discovered in November 2007 in an outbreak in Bundibugyo
district, near the border of Uganda and Congo (Kinshasa); it causes death in
about 25 percent of cases.
Outbreaks
The first outbreaks in 1976 in Zaire (now Congo [Kinshasa]) and The Sudan
resulted in more than 400 deaths. A subsequent outbreak in Congo (Kinshasa) in
May 1995 prompted temporary quarantine of the Kikwit region, and more than
250 people died. Later outbreaks in Uganda
in 2000 and in Congo (Kinshasa) in 2002 also resulted in several hundred
deaths. In September 2007 an outbreak was confirmed in Congo (Kinshasa) in the
Kasai-Occidental (West Kasai) province, located in the south-central region of
the country. However, while Ebola was detected in blood samples from some
people that fell ill, other people were found to be infected with Shigella, the bacterium that causes dysentery—a disease whose symptoms are
similar to the early symptoms of Ebola. As a result, although several hundred
people became ill and more than 160 people died during the Ebola outbreak, it
was unclear how many of the deaths were actually caused by Ebola. Less than two
years later, in December 2008, a second outbreak of the disease was confirmed
in the Kasai-Occidental province. Ebola had been detected in just four people
by early 2009; however, another 42 cases were suspected, and some 200 people
were under close observation for infection. Although 13 deaths had been
reported in association with the outbreak, samples collected from the victims
did not test positive for Ebola.
In 2008, tissue samples from pigs that died of unknown
causes in the Philippines were analyzed and found to contain Ebola-Reston
virus. This was the first time that the virus was found in a mammalian species
other than primates. Infections in pigs were unexpected and raised concerns
about transmission of the virus from pigs to humans. In January 2009, antibodies to Ebola-Reston were found in five
Filipinos, four of whom worked on pig farms and one of whom worked in a
slaughterhouse. All five individuals were believed to have been infected with
the virus through direct contact with infected pigs. The infected people were
healthy and did not show signs of infection at the time antibodies to the virus
were detected. In order to stop the spread of Ebola-Reston among pigs,
Philippines officials authorized the slaughter of thousands of potentially
infected swine.
However in April 2014, most part of Western Africa was visited by Ebola virus, but this time the virus did not only affected West African countries but other countries outside Africa. It was reported that two US doctors were infected with the virus and they were treated. The Ebola virus this time around affected West African countries like Nigeria and Ghana, the virus was reported to have been brought into Nigeria by a Librarian statesman known as Patrick Sawyer. This action can be regarded as a bio-terrorist act, as Mr Patrick who is now deceased is said to have knowingly brought the virus to the Nigerian state, as he was reported to have been avoiding treatment and urinating on other patient in the Obalende Hospital in Lagos State. Also, just in September 2014, the U.S. Centers for Disease Control and Prevention recorded its first ever Ebola patient, Eric Duncan, who is said to be from Dallas and in critical condition. Reports has it that about 10 people are at "higher risk" of catching Ebola after coming into contact with Duncan but have shown no symptoms, health officials said Saturday. The group is among 50 people being monitored daily, but the other 40 are considered "low risk," said Dr. David Lakey, the commissioner of Texas department of state health services.
However in April 2014, most part of Western Africa was visited by Ebola virus, but this time the virus did not only affected West African countries but other countries outside Africa. It was reported that two US doctors were infected with the virus and they were treated. The Ebola virus this time around affected West African countries like Nigeria and Ghana, the virus was reported to have been brought into Nigeria by a Librarian statesman known as Patrick Sawyer. This action can be regarded as a bio-terrorist act, as Mr Patrick who is now deceased is said to have knowingly brought the virus to the Nigerian state, as he was reported to have been avoiding treatment and urinating on other patient in the Obalende Hospital in Lagos State. Also, just in September 2014, the U.S. Centers for Disease Control and Prevention recorded its first ever Ebola patient, Eric Duncan, who is said to be from Dallas and in critical condition. Reports has it that about 10 people are at "higher risk" of catching Ebola after coming into contact with Duncan but have shown no symptoms, health officials said Saturday. The group is among 50 people being monitored daily, but the other 40 are considered "low risk," said Dr. David Lakey, the commissioner of Texas department of state health services.
Course of infection
Viewed through an electron microscope, the Ebola virus
appears as long filaments, sometimes branched or intertwined. The virion (virus
particle) contains one molecule of noninfectious, single-stranded RNA (ribonucleic acid). It is not known
how the Ebola virus attacks cells; however, it has been postulated that the
virus produces proteins that suppress the immune
system, allowing
reproduction of the virus to continue unhindered. Viral hemorrhagic fevers
similar to Ebola typically are carried by arthropods and rodents; however, the
natural reservoir for the Ebola virus has yet to be discovered. Among the
suspected reservoirs for Ebola are bats, primates, rodents, and insects that
inhabit tropical forests in Africa and Asia. Ebola can be transmitted through
contact with infected blood, bodily fluids, and possibly respiratory
secretions. The virus has also been detected in the organs of patients after recovery
from the fever. Unsanitary conditions and lack of adequate medical supplies may
be factors in the spread of the disease.
The Ebola virus has an incubation period of 4 to 16
days. The onset is sudden and harsh. Infected persons develop fever, severe
headaches and muscle aches, and loss of appetite. Within a few days the virus
causes a condition known as disseminated
intravascular coagulation, which is marked by both blood
clots and hemorrhaging. In the case of Ebola fever, clots are concentrated in
the liver, spleen, brain, and other internal organs, forcing capillaries to
bleed into surrounding tissue. Nausea, vomiting and diarrhea with blood and
mucus, conjunctivitis, and sore throat soon follow. A
maculopapular rash (discoloured elevations of the skin) appears on the trunk
and quickly spreads to the limbs and head. The patient is then beset by
spontaneous bleeding from body orifices and any breaks in the skin, such as
injection sites, and within the gastrointestinal tract, skin, and internal organs.
Death is usually brought on by hemorrhaging, shock, or renal failure and occurs within
8 to 17 days.
Treatment
There is no known treatment for Ebola fever, although
immune plasma may be beneficial. Current therapy consists of maintenance of
fluid and electrolyte balance and administration of blood and plasma to control
bleeding.
Drugs designed to disrupt Ebola virus replication have
been developed and tested in Ebola-infected monkeys. One such therapy was found
to protect more than 60 percent of rhesus
monkeys infected
with Ebola-Zaire when the agent was administered within 30 to 60 minutes
following infection. The treatment, which in 2010 was approved for safety
trials in humans, was promising for persons who become accidentally infected in
laboratory or hospital settings.
The spread of Ebola virus can be contained by barrier
nursing, handling of infected blood and tissue in isolated laboratory units,
and proper decontamination of reusable equipment. Keep save and spread the
message not the virus.
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Reference and Credit:
"Ebola." Encyclopædia
Britannica. Encyclopædia Britannica Ultimate Reference Suite.
Chicago: Encyclopædia Britannica, 2012.
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