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WASHINGTON,
June 6, (Rtr): Using protective balls of fat and precisely
targeted antibodies, researchers said on Monday they had found
a way to sneak gene therapy into the brain in a new approach
they hope could be used against a range of diseases from Alzheimer's
to brain cancer.
They
said their new method might also be used in general as a safe
and effective technique for gene therapy of all kinds.
And,
although they did their work in ratS, they think their technique
might be ready to be tested in humans within months.
Dr
William Pardridge, a professor at the University of Califomia
LOs Angeles School of Medicine, said gene therapy has not
worked weUinthe past and attempts to make it work in the brain
have been especially un- successful.
"The
reason all pharmaceutical companies have given up on gene
therapy of the brain is it requires drilling a hole in your
head that's expensive, invasive and it doesn'twork," Pardridge
said in a telephoneinteryiew."
"The
gene only goes to apart of your brain the size of a pin head.
The second problem is they uhiformly use viruses, either adeno-Viruses
or herpes viruses, and we all have a pre- existing immunity
to either virus."
The
idea behind gene therapy is to correct disease or genetic
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defects
by introducing new genes into the body. It is still highly
experimental and the field suffered a setback last year when
one patient died, apparently because his immune system revolted
against the virus used to carry the genes.
Writing
in the Proceedings of theNational Academy of Sciences, Pardridge's
team said they had taken another standard gene therapy route,
using capsules of fat known as liposomes.
To
target the liposomes, they attached antibodies, which are
immune system compounds that can seek out and attach to specific
cells, as well as viruses and bacteria.
This
enables us one, to have wide-spread distribution and expression
o the gene through the brain following a simple intravenous
injection and two, no use of viruses, " Pardridge said.
"The
DNA is encapsu-lated from the liposome so it is fully protected
from all the enzymes that are there to chew it up."
But
just injecting DNA is no good, because it does know where
to go. That is where the antibodies come in.
Pardridge's
team used as their target the transferrin receptor, which
is a molecule found on brain cells and on cells in certain
other organs such as the liver.
Gene
therapy in the
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brain
might be used to treat or even cure Parkinson's disease, brain
cancer and genetic disorders such as Tay-Sachs and Gaucher's
disease. Pardridge thinks the approach could be used against
a range of other disease, too.
"You
can deliver any thing you want to cells," he said. "It
opens up an entirely new approach to pharmaceutics."
But
what was especially intriguing about this approach, he said,
was it was able to get past the "blood-brain barrier"
- a molecular system that keeps many drugs from getting into
brain cells.
"Now
we have found a way to ferry genes across the barrier by exxploiting
natural receptors in the brain."
Pardridge
hopes his team can move ahead quickly.
"The
next step is usually you say three to five years.
before
studies in humans," he said. "That isn't the case
here."
He
said his team had a project that could move into human beings
within five months.
But,
he said, no drug companies were interested.
"All
of the components are available off the shelf now, but who
is going invest in this?" he asked. "It's a problem.
You mention blood-brain barrier to venture capitalists and
thier eyes get glazed over."
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