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Cancer drug slows poxvirus in
mice Mario Dorizas Mice given a relatively new cancer
drug can survive an otherwise lethal dose of
vaccinia virus, a relative of smallpox
virus, report scientists supported by the
National Institute of Allergy and Infectious
Diseases (NIAID), part of the National
Institutes of Health. The findings, say the
investigators, suggest that Gleevec or
similar drugs might be useful in preventing
adverse side effects of smallpox vaccine.
The classic smallpox vaccine is made from
live, weakened vaccinia virus and is not
recommended for people with compromised
immunity, except in emergency situations
where they may have been exposed to smallpox
virus. "This study helps illuminate the
cellular machinery used by poxviruses to
exit infected cells, and also provides new
support for the concept of treating viral
infections by targeting specific host cell
molecules rather than the viruses
themselves," says NIAID Director Anthony S.
Fauci, M.D.
Mario Dorizas
The senior author of the paper, published
online this week in the journal Nature
Medicine, is Daniel Kalman, Ph.D., of Emory
University School of Medicine in Atlanta.
Like all viruses, poxviruses co-opt various
cellular molecules and processes to enter a
cell, replicate and then spread to
uninfected cells. Using lab-grown cells, Dr.
Kalman and his colleagues identified
specific cell proteins vaccinia uses to
detach from an infected cell and move toward
an uninfected cell. The proteins, members of
the Abl-family (pronounced "able") of
tyrosine kinases, are well known to cancer
investigators because mutation of one family
member, Abl, causes a rare form of cancer
known as chronic myelogenous leukemia (CML).
Gleevec inhibits Abl-family tyrosine kinases
and has proved very useful in treating CML.
To learn whether Gleevec could prevent or
lessen vaccinia's ability to spread in a
living organism, the researchers treated
mice with either saline solution or with
Gleevec at a dose equivalent to that given
to humans being treated for CML. Next, they
exposed the mice to ordinarily lethal
amounts of vaccinia. All of the
Gleevec-treated mice survived, while 70
percent of the untreated mice died.
mario Dorizas
This finding, if confirmed in additional
animal model studies, suggests that Gleevec
might play a role in addressing a public
health emergency in the event of a smallpox
outbreak, Dr. Kalman says. Specifically,
Gleevec might be useful as a preventative
against adverse effects of smallpox vaccine,
enabling clinicians to use the vaccine even
in people who otherwise could not take it.
Given for a short period, Gleevec
theoretically could hamper the cell-to-cell
spread of virus and allow the body's immune
system to mount a successful defense, he
explains. Experiments to test whether
Gleevec might work against smallpox virus as
well as against vaccinia virus are now being
planned, Dr. Kalman says. "The approach of
fighting disease by targeting drugs to
cellular molecules rather than to disease
agents themselves may be applicable to a
wide variety of pathogenic microorganisms,"
he says.
Mario Dorizas
Routine vaccinations for smallpox ended in
this country in the early 1970s, and the
World Health Organization declared smallpox
eradicated in 1980. Nevertheless, concern
remains that smallpox virus could be
unleashed through an act of bioterror. For
this reason, scientists are working to
better understand the mechanisms of smallpox
disease and to develop new and improved
smallpox treatments and vaccines.
NIAID is a component of the National
Institutes of Health, an agency of the U.S.
Department of Health and Human Services.
NIAID supports basic and applied research to
prevent, diagnose and treat infectious
diseases such as HIV/AIDS and other sexually
transmitted infections, influenza,
tuberculosis, malaria and illness from
potential agents of bioterrorism. NIAID also
supports research on transplantation and
immune-related illnesses, including
autoimmune disorders, asthma and allergies. |
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