The
World Health Organization (WHO) said on Friday it expected to begin small-scale
use of two experimental Ebola vaccines in West Africa early next year and in
the meantime, transfusions of survivors' blood may offer the best hope of
treatment, Reuters reports.
WHO is working with pharmaceutical companies and
regulators to accelerate the use of a range of potential treatments to fight
the disease that has no cure and which has killed 2,917 out of 6,263 people
infected in West Africa since an outbreak began in March, a senior WHO official
said.
GlaxoSmithKline has begun clinical trials of its
vaccine in the United States and Britain, to be followed by a trial starting in
Mali next week, while NewLink vaccine trials are about to start in the United
States and Germany, said Dr. Marie-Paule Kieny, WHO assistant director-general.
"If everything goes well again we might be able
to start to use some of these vaccines in affected countries at the very
beginning of next year, in January. This will not be a mass vaccination
campaign, let's be clear about that because the quantity which will be
available doesn't make this possible," Kieny told a news briefing in
Geneva.
She stressed however that the shots are experimental
and have not yet been shown to work against Ebola: "They have given very
promising results in monkeys, but monkeys are not humans.
"We could still face a situation where these
vaccines would be unsafe in humans or where they would do nothing in terms of
protection. So we need to be very prudent."
Data will be collected from clinical trials when the
experimental vaccines are being given to healthy volunteers who are then
monitored for adverse side effects and to see if the shot elicits an immune
response in their blood.
Regulators at the European Medicines Agency (EMA) said
on Friday they would begin reviewing data on experimental Ebola medicines to
support any decisions made on whether to use them for treating patients.
And the global vaccines alliance GAVI - the world's
biggest funder of immunizations for people in poor countries - said in a
statement that it was exploring how it could help speed up the availability of
any Ebola vaccines that prove effective.
Canada has given 800 vials of the NewLink candidate
vaccine to WHO, expected to yield at least 1,500 doses, Kieny said, and the
U.S.-based firm is "working very hard to produce a few more thousand doses
in the coming months," she said.
GSK has said it hopes to have 10,000 doses of its
experimental vaccine by the end of this year.
Kieny said an experimental Ebola vaccine being
developed by Johnson & Johnson but not yet ready for trials in humans is
also under consideration.
ZMAPP DOSES BY
YEAR-END
Experimental Ebola drugs including compounds from
Mapp Biopharmaceutical, Sarepta and Tekmira will be tested in affected states
for the first time in a bid to fast-track trials, the Wellcome Trust said on
Tuesday.
WHO is taking part in that effort, Kieny said.
"We are starting to discuss with African sites to see which would be the
most suitable to test these new drugs and establish as soon as possible which
one gives an advantage for survival to patients."
ZMapp has been used to treat several Ebola patients
who have since recovered, but doctors cannot say for sure whether the drug
helped them or whether they would have recovered anyway.
"In terms of ZMapp, the best as we have known for
a few weeks now, is that maybe a few hundred doses will be available by the end
of the year. But clearly this is not the kind of scale that can have impact on
the epidemic curve," Kieny said of the drug by the California-based
private biotech firm.
The use of blood transfusion and infusion of human
serum from Ebola survivors is recognized as a "safe treatment", but
donated blood must be screened for infections including HIV and hepatitis, she
said.
There was only anecdotal information on its use in
Ebola-infected healthcare workers, as there
is no system in place.
"Will it be efficacious? For the time being we
don't know because there are not enough people who have been treated,"
Kieny said, adding that they could be counted on two hands.
"This
is something where the African population doesn't have to wait for anybody else
to develop it for them. This is why there is a lot of enthusiasm," Kieny
said.
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