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Can cancer tumors be starved to death?
Thousands of cancer patients are clamoring this week to
be among the 30 or so enrolled in a new and controversial
trial designed to seek an answer to this question. One of
the most exciting and frustrating things about watching
a developing science story like this one is that you can't
flip ahead and read the ending -- in the real world of scientific
research, you never know how things are going to turn out.
The saga of Judah Folkman is very much that kind of story.
Dr. Folkman, a Harvard researcher, is a pioneer in efforts
to cure cancer by starving tumors to death. Dr. Folkman's
research follows up on a familiar observation made by many
oncologists (cancer specialists), that removal of a primary
tumor often lead to more rapid growth of secondary tumors.
"Perhaps," Folkman reasoned, "the primary
tumor is producing some substance that inhibits the growth
of the other tumors." Such a substance could possibly
be a powerful weapon against cancer.
Folkman set out to see if he could isolate a chemical from
primary tumors that inhibited the growth of secondary ones.
Two years ago he announced he had found not one, but two.
He called them angiostatin and endostatin.
To understand how these two proteins work, put yourself
in the place of a tumor. To grow, a tumor must obtain from
the body's blood supply all the food and nutrients it needs
to make more cancer cells. To facilitate this necessary
grocery shopping, tumors leak out substances into the surrounding
tissues that encourage angiogenesis, the formation of small
blood vessels. This call for more blood vessels insures
an ever-greater flow of blood to the tumor as it grows larger.
When examined, Folkman's two cancer inhibitors turned out
to be angiogenesis inhibitors. Angiostatin and endostatin
kill a tumor by cutting off its blood supply. This may sound
an unlikely approach to curing cancer, but think about it
-- the cells of a growing tumor require a plentiful supply
of food and nutrients to fuel their production of new cancer
cells. Cut this off, and the tumor cells die, literally
starving to death.
By producing factors like angiostatin and endostatin, the
primary tumor holds back the growth of any competing tumors,
allowing the primary tumor to hog the available resources
for it's own use.
In tests in his laboratory, Folkman's anti-tumor factors
caused tumors in mice to regress to microscopic size, a
result that electrified researchers all over the world.
Other scientists were soon trying to replicate this exciting
result. Some succeeded, while others did not. Five major
laboratories have made their own endostatin and published
their findings of antitumor activity, but other researchers
have reported difficulty in repeating the successful tests.
National Cancer Institute scientists have replicated Folkman's
results while working in his lab, but failed to get the
same results when they went back to their own laboratory.
Why the variability? Purifying finicky
natural products in a way that retains their activity can
be notoriously difficult. When you don't know much about
the requirements of the factor you are isolating, it can
be like grasping smoke.
For example, what if Folkman's anti-tumor factors turn out
to be zinc proteins (that is, they require trace amounts
of the metal zinc in order to be active, as many enzymes
in the human body do). A little zinc in Folkman's laboratory
water supply -- say, the amount in ordinary tap water --
might be all that would be required to keep the factors
active during the isolation process. Researchers working
at The National Cancer Institute, with its ultra-pure zinc-free
water, simply might not be supplying the anti-tumor factors
the traces of zinc they require.
I don't think anyone really knows why the isolation works
sometimes and not others. That it works at all seems to
me the key take-home lesson.
Last month, Folkman announced the isolation of yet a third
angiogenesis inhibitor. It is even more potent in reducing
blood vessel formation and in shrinking tumors, Folkman
claims.
The National Cancer Institute is proceeding with tests of
Folkman's factors in humans, a decision criticized this
month by the Wall Street Journal as overhasty, because full-scale
animal trials have not been successfully completed.
To me, the NCI decision to proceed directly to human tests
seems fully warranted. Human endostatin has been shown to
be "completely and utterly safe," and it clearly
has efficacy against mouse tumors. We will learn a lot sooner
if this stuff works by proceeding right to human trials,
without spending years sorting out the variability of animal
trial results. Either we have a powerful new weapon against
cancer, or we don't. Its time to ask -- and answer -- that
question.
http://www.txtwriter.com/
onscience/Articles/angiogenesis.html
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