IS THERE AN EFFECTIVE TREATMENT FOR EBOLA
A leading U.S. Ebola
researcher from the University of Texas Medical Branch at Galveston has gone on
record stating that a blend of three monoclonal antibodies can completely
protect monkeys against a lethal dose of Ebola virus up to 5 days after
infection, at a time when the disease is severe.
Thomas Geisbert,
professor of microbiology and immunology, has written an editorial for Naturediscussing
advances in Ebola treatment research. The filoviruses known as Ebola virus and
Marburg virus are among the most deadly of pathogens, with fatality rates of up
to 90 percent.
Since the discovery of
Ebola in 1976, researchers have been actively working on treatments to combat
infection. Studies over the past decade have uncovered three treatments that
offer partial protection for monkeys against Ebola when given within an hour of
virus exposure. One of these treatments, a VSV-based vaccine was used in 2009
to treat a laboratory worker in Germany shortly after she was accidentally
stuck with a needle possibly contaminated by an Ebola-infected animal.
Further advances have
been made that can completely protect monkeys against Ebola using small
'interfering' RNAs and various combinations of antibodies. But these treatments
need to be given within two days of Ebola exposure.
"So although
these approaches are highly important and can be used to treat known exposures,
the need for treatments that can protect at later times after infection was
paramount," said Geisbert.
Further research led
to a cocktail of monoclonal antibodies that protected 43% of monkeys when given
as late as five days after Ebola exposure, at a time when the clinical signs of
the disease are showing.
The new study from Qui
and colleagues at MAPP Biopharmaceutical Inc. used ZMAPP to treat monkeys given
a lethal dose of Ebola. All of the animals survived and did not show any
evidence of the virus in their systems 21 days after infection, even after
receiving the treatment 5 days after infection. They also showed that ZMAPP
inhibits replication of the Ebola virus in cell culture.
ZMAPP has been used to
treat several patients on compassionate grounds. Of these, two US healthcare
workers have recovered, although but whether ZMAPP had any effect is unknown,
as 45% of patients in this outbreak survive without treatment. There were also
two patients treated with ZMAPP who did not survive, but this may be because
the treatment was started too late in the disease course.
"The diversity of
strains and species of the Ebola and Marburg filoviruses is an obstacle for all
candidate treatments," said Geisbert. "Treatments that may protect
against one species of Ebola will probably not protect against a different
species of the virus, and may not protect against a different strain within the
species."
Although we certainly
need treatments for filovirus infections, the most effective way to manage and
control future outbreaks might be through vaccines, some of which have been
designed to protect against multiple species and strains. During outbreaks,
single-injection vaccines are needed to ensure rapid use and protection. At
least five preventative vaccines have been reported to completely protect
monkeys against Ebola and Marburg infection. But only the VSV-based vaccines
have been shown to complete protect monkeys against Ebola after a single
injection.
"Antibody
therapies and several other strategies should be included in the arsenal of
interventions for controlling future Ebola outbreaks," said Geisbert.
"Although ZMAPP in particular has been administered for compassionate use,
the next crucial step will be to formally assess its safety and
effectiveness."
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