St. Jude develops vaccine against potential pandemic influenza
virus H5N1 using reverse genetics
Special modification of reverse genetics created at St.
Jude allowed vaccine to be custom-made within weeks of emergence of virus
(MEMPHIS, TENN.--April 2, 2003) Scientists at St. Jude Children's Research
Hospital announced today the development of a vaccine against H5N1, a new lethal
influenza virus that triggered the World Health Organization (WHO) to declare a
pandemic alert in February 2003.
The virus appeared in birds in Hong Kong late last year and subsequently
killed one of two infected people with rapidly progressive pneumonia in the past
month. St. Jude developed the vaccine in only four weeks from the time it
received the H5N1 sample from colleagues in Hong Kong.
The announcement comes at a time when a second, as-yet-unidentified virus,
has taken several lives around the world. The unknown virus, which causes severe
acute respiratory syndrome (SARS), appears to have originated at the same time
and in the same place as the new "flu."
The development of the initial ("seed") batch of H5N1 vaccine is significant
because humans do not have a natural immunity to the virus, according to Robert
Webster, Ph.D., a member of the Department of Infectious Diseases at St. Jude.
Rather, humans appear to become infected through contact with chickens and other
birds. In the past the virus killed only the chickens it infected. But the new
variant of H5N1 also killed many kinds of wild birds, which is unusual.
If H5N1 acquires the ability to pass from human to human, there would be the
potential for concern similar to that for SARS, according to Webster.
"It's likely there were two things that prevented the 1997 poultry influenza
outbreak in Hong Kong from becoming more deadly--its inability to spread from
human to human and the slaughter of more than 1.5 million chickens and other
birds in the open-air markets of Hong Kong, which eliminated the source of the
virus," Webster said. "In fact, the sudden appearance of SARS in the same region
of the world is just another warning that the large populations of people and
poultry in this region are a potential source of viruses."
Webster is the director of the WHO's U.S. Collaborating Center at St. Jude
that studies animal influenza viruses. It is the only WHO laboratory that
focuses on the transmission of animal viruses to humans.
Webster's laboratory has sent the seed H5N1 vaccine to the Centers for
Disease Control in Atlanta and the World Influenza Center in London for further
testing, in preparation for initial Phase I and Phase II trials in humans. "It's
important to move right along with these trials in case the virus begins
spreading from person to person," Webster says. Led by Richard Webby, Ph.D., and
Daniel Perez, Ph.D., the St. Jude laboratory team successfully modified a
technique called reverse genetics to permit them to develop the H5N1 vaccine so
quickly. Using the samples of H5N1 obtained from Hong Kong, Webby mixed two
genes from H5N1 with six genes from a second virus (A/PR8/34)[H1N1]). H1N1 is a
rapidly growing "master" strain of virus commonly used to make vaccines.
The genes from flu viruses produce proteins called HA and NA, which are on
the surface of the virus, in full "view" of the immune system. Webby took the
modified gene for HA and the NA from H5N1 and mixed them inside a cell with six
genes from H1N1. The HA gene was modified to abolish its ability to cause
disease and therefore made it safer to use in the vaccine.
The genes mixed together, and the resulting vaccine virus produced in the
cell thus carried HA and NA from H5N1. But because of the alterations to the HA,
and the rest of the genes being derived from H1N1, the new virus vaccine cannot
cause disease. Rather, it can only stimulate the immune system to respond to
H5N1.
"The St. Jude vaccine is like a gun without ammunition," said Elaine Tuomanen,
M.D., director of the St. Jude Department of Infectious Diseases. "The vaccine
looks deadly enough for its HA and NA proteins to alert the immune system. But
in reality, it's carrying blanks that can't cause disease."
Key to the quick success in developing the vaccine was the on-campus
availability of GMP (Good Manufacturing Practices) facilities, which are
equivalent in quality to those used by pharmaceutical companies to make
biological agents such as vaccines. In addition, the centralization of genetic
analysis and other molecular biology work, performed in the Hartwell Center for
Bioinformatics and Biotechnology at St. Jude, greatly accelerated the process of
building the vaccine components.
"We've been lucky twice with H5N1--once in 1997 and once so far during this
current outbreak--in not experiencing human-to-human transmission," Webster
says. "But the mixing bowl in Hong Kong is still stirring up new variations of
familiar viruses. Although we just made a vaccine against one of that mixing
bowl's nasty viral brews, SARS shows us there's always another threat down the
road."
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St. Jude Children's Research Hospital St. Jude Children's Research Hospital,
in Memphis, Tennessee, was founded by the late entertainer Danny Thomas. The
hospital is an internationally recognized biomedical research center dedicated
to finding cures for catastrophic diseases of childhood. The hospital's work is
supported through funds raised by ALSAC. ALSAC covers all costs not covered by
insurance for medical treatment rendered at St. Jude Children's Research
Hospital. Families without insurance are never asked to pay. For more
information, please visit http://www.stjude.org.
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