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Ed. Note: The following is a press release issued by the National
Institutes of Health.
Monday, May 3, 2004
Researchers may be on the trail of a new and more targeted treatment for
severe chronic pain. In the current issue of the Journal of Clinical
Investigation, a team of scientists established in a series of animal
studies the therapeutic potential of selectively deleting specific nerve
cells from the nervous system that convey severe chronic pain.
So effective was the treatment in eight dogs severely affected by
osteroarthritis, cancer-related pain, or both, all eventually became more
active and later walked with slight or no limps. Just as importantly, none
showed any adverse side effects from the treatment, their temperaments were
improved, and their need for other pain-controlling medications was
eliminated or greatly reduced.
The authors also reported selectively deleting the nerve cells, called
C-fiber neurons, from among various human neurons cultured together in the
laboratory, an indication the strategy might work in people. C-fibers convey
to the central nervous system sensations of noxious heat and certain
inflammatory signals. "Some have referred to the technique as using a
'molecular scalpel,'" said Dr. Michael J. Iadarola, a scientist at the NIH's
National Institute of Dental and Craniofacial Research (NIDCR) and a senior
author on the paper. "The technique selectively deletes certain neurons but
leaves others untouched. As a result, the nervous system functions normally,
it's just a certain spectrum of pain responsiveness that has been deleted."
Currently, doctors have no way of selectively eliminating nerve cells
involved in chronic pain. Opioid-based analgesics, the mainstay of current
treatments for moderate to severe chronic pain, cannot provide universal
relief, and other treatments are nonselective and/or can cause serious side
effects.
Iadarola said this month's paper stems from using the old drug
resiniferatoxin, or RTX, in a new way. First isolated in the 1970s, RTX is
often used as a laboratory tool because of its ability to bind to a
much-studied protein called vanilloid receptor 1 (VR1), which is displayed
on the surface of certain types of heat-pain-sensing neurons. As several
laboratories have reported previously, RTX attaches to VR1, and, like
opening a window, prompts a brief influx of calcium through a channel, or
pore, but only in those cells that manufacture the ion channel.
Three years ago, Iadarola's group published data showing the RTX-induced
flow of calcium can overdose, seriously disable, and ultimately kill these
neurons. Because nerve cells in the peripheral nervous system first transmit
their signals to the spine, where they then are processed and routed onward
to the brain, their previous finding raised an intriguing therapeutic
scenario: The cell bodies of these peripheral neurons bundle together in
groups near the spine, called dorsal root ganglia. If RTX were applied
directly to the ganglia, the scientists knew that they could selectively
delete specific neurons, such as C-fibers, that express large amounts of the
VR1 protein on their surface. By doing this, they wondered whether they
could also permanently turn off their chronic pain signals, which are
involved in severe arthritis, peripheral neuromas, trigeminal neuralgia, and
advanced cancer?
"We realized that by focusing on RTX's ability to kill cells, we could apply
it therapeutically," said Dr. Laszlo Karai, an NIDCR scientist and lead
author on the paper. "That might seem like a radical departure from the
standard paradigm of blocking protein receptors or desensitizing them to
control pain, but our laboratory data, obtained from cells in a dish, was so
compelling that we thought it just might work."
As reported this month, Karai et al. performed a series of experiments in
rats that showed a single injection into the trigeminal ganglion (supplies
sensation to the face), or into the cerebrospinal fluid that bathes the
dorsal root ganglia, (supply sensation to the body), most likely deleted the
C-fiber neurons permanently. The same held true when they injected the drug
into multiple ganglia that connect to the tail and hind legs. In both
experiments, rats maintained their normal motor function as well as their
ability to respond to other sensory stimuli, such as warm and very hot
thermal stimulation and a mechanical pinch, an indication that RTX had only
affected C-fiber neurons.
"This showed us that the deficit in terms of overall pain sensation was
probably minimal," said Dr. Zoltan Olah, an NIDCR scientist and one of the
inventors of the technology. "What was lost were the C-fiber neurons, which
confer that sense of aching, chronic pain."
The group then applied the technique to dogs, whose owners had brought them
into nearby veterinary hospitals with severe pain from arthritis and cancer.
"We were very encouraged to see a long-term therapeutic benefit that did not
diminish with the progression of the disease," said Iadarola. "When a cancer
progresses, you often have to increase the dose of conventional pain
medications, such as opiate analgesics, which can produce alterations of
consciousness, activity level, and other severe side effects that can impair
overall quality of life."
Based on these data, Iadarola said the RTX technique has tremendous
potential in veterinary care. But the group's ultimate goal is to move the
treatment into early stage clinical trials in the near future for people
with severe chronic pain. "One reason we were successful is we have a
vertically integrated, multipdisciplinary group," said Iadarola. "There is a
molecular/cell biologist, a pharmacologist, an anaesthesiologist, and a
pathologist. We realized that permanently deleting cells wasn't a farfetched
concept, and, if we applied this approach correctly, we could get it to
work. And, that's what happened."
The study is titled, "hDeletion of vanilliod receptor 1-expressing primary
afferent neurons for pain control." It is published in the May 2004 issue of
The Journal of Clinical Investigation. The authors are: Laszlo Karai,
Dorthothy Brown, Andrew J. Mannes, Stephan T. Connelly, Jacob Brown, Michael
Gandal, Ofer W. Welisch, John K. Neubert, Zoltan Olah, and Michael J.
Iadarola. All are affiliated with NIDCR, except Dr. Brown, who is in the
School of Veterinary Medicine at the University of Pennsylvania.
CONTACT:
Bob Kuska
301-594-7560
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