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Archive Number 20020312.3728
Published Date 12-MAR-2002
Subject PRO/AH> West Nile virus, candidate human vaccine (02)
WEST NILE VIRUS, CANDIDATE HUMAN VACCINE (02)
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A ProMED-mail post
<http://www.promedmail.org>
ProMED-mail is a program of the
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[see also:
West Nile virus, candidate human vaccine 20020306.3695
West Nile virus, goose vaccine           20020206.3493
2001
----
West Nile virus, equine vaccine          20010804.1533
West Nile virus, equine vaccine (02)     20010808.1867
West Nile virus, vaccine research        20010607.1117]

Date: Tue 12 Mar 2002
From: ProMED-mail <promed@promedmail.org>
Source: Newsday.com, Tue 12 Mar 2002 [edited]
<http://www.newsday.com/news/health/ny-dsbelow2621105mar12.story?coll=ny%2Dh
ealth%2Dheadlines>


Alternate Route to a Hybrid West Nile virus Vaccine
---------------------------------------------------
In the race for an effective vaccine against West Nile virus, 2 independent 
research teams have taken similarly promising pathways toward the finish 
line. In both efforts, scientists swapped genes from the potentially fatal 
West Nile virus into the "backbone" genome of a distantly related virus. 
Researchers have reached 2 main conclusions with the resulting vaccines 
created by using the hybrid viruses: They are dramatically weakened, but 
they protect laboratory animals against lethal doses of the West Nile 
strain that first swept across the New York region in 1999.

The most recent research, published last week in the Proceedings of the 
National Academy of Sciences, details the efforts of scientists from the 
National Institute of Allergy and Infectious Diseases in Bethesda, MD and 
Walter Reed Army Institute of Research in Silver Spring, MD. The 
collaborators spliced 2 genes for West Nile coat proteins into a dengue 
virus backbone stripped of its own corresponding genes. West Nile virus and 
dengue virus belong to the flavivirus family of tick- and mosquito-borne 
viruses, a family that also includes yellow fever virus and Japanese 
encephalitis virus. [This research was summarised previously in the 
ProMED-mail post archived as "West Nile virus, candidate human vaccine 
20020306.3695". - Mod.CP]. Dr. Robert Chanock, a senior investigator and 
mentor to the Infectious Diseases Institute coauthors, stated that the 
hybridization process between these distantly related viruses greatly 
reduces the amount of replicating hybrid virus, but allows enough of it to 
reproduce so that its coat proteins can induce a strong protective immune 
response against West Nile virus.

Thomas Monath, a vice president at the vaccine development company Acambis 
in Cambridge, MA, called the report an "excellent study," but he cautioned 
that the research is still in its early stages. Monath's company has taken 
a similar approach to developing a West Nile virus vaccine, by swapping the 
same 2 West Nile virus genes into the backbone genome of [an attenuated] 
yellow fever virus. Monath said that researchers currently have much more 
experience with the yellow fever virus backbone, which they've used to 
successfully present the West Nile virus coat proteins to animal immune 
systems. Acambis has already demonstrated that its hybrid vaccine protects 
horses and primates from West Nile virus infection, he said, including 
current trials with rhesus monkeys and baboons. The company hopes to start 
human clinical trials by this summer.

Acambis has already completed 3 human clinical trials using a hybrid 
vaccine with a yellow fever virus backbone and genes for the coat proteins 
of Japanese encephalitis virus, a close relative of West Nile virus. Monath 
said the latest of these trials, reported in the January issue of the 
journal Vaccine, was a "spectacular success. If we can do it for Japanese 
encephalitis, we're very confident we can do it for West Nile."

[Byline: Bryn Nelson]

--
ProMED-mail
<promed@promedmail.org>

[In accordance with the standard policy of ProMED-mail to avoid comment on 
vaccines under development, this thread is now cut until the results of the 
projected human trials for both vaccines become available. - Mod.CP]
..............................cp/pg/es
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