Pubdate: Fri, 13 Aug 2004 Source: StarPhoenix, The (CN SN) Copyright: 2004 The StarPhoenix Contact: http://www.canada.com/saskatoon/starphoenix/ Details: http://www.mapinc.org/media/400 Author: Betty Ann Adam POT STUDY OFFERS SURPRISE Marijuana researchers have found that a component of pot may intensify the severity of the most common type of epileptic seizures. The finding was a surprise for research group leader Dr. Michael Corcoran at the University of Saskatchewan, who said this week he expected findings would support older research that had suggested high doses of THC, the psychoactive ingredient of cannabis, could suppress grand mal-type seizures. Now, Corcoran suspects the effects of THC or its synthetic form, known as cannabinoids, may depend on the part of the brain where the seizure occurs. The regions of the brain that are susceptible to epilepsy are mainly those involved in learning and memory, he said. Corcoran's experiments on rats have shown that seizures which begin in the temporal lobes appear to last longer and be more severe after cannibinoids are administered. He thinks studies conducted in the 1980s, which suggested some seizures may be suppressed by marijuana, may have been looking at grand mal seizures that begin in a different part of the brain, the brain stem. Research conducted in the past decade has found that there are at least two, possibly three, different types of receptors in the body for marijuana-like compounds, including some on nerve cells. These "cannabinoid receptors" normally are acted upon by various naturally occurring marijuana-like substances called "endogenous cannabinoids." One of those endogenous cannabinoids has been aptly labelled andomide, a term derived from the Sanskrit word meaning bliss, Corcoran noted. Identifying and cloning the receptor allowed researchers to design artificial drugs that act very selectively at that receptor, to turn it on or block the action of cannabinoids, Corcoran said. Using a process called kindling, Corcoran gradually induces epilepsy in rats by administering low doses of electricity to the brain. Once epilepsy has been induced, the brain becomes more susceptible to seizures than a normal brain. Corcoran found that administering cannabinoids before kindling caused rats to develop epilepsy much sooner than those that didn't get the marijuana component. "It's really completely the opposite of what I expected," he said. "Instead of finding potentially useful anti-epileptic effects, we found the opposite." Still, Corcoran is not saying people who smoke pot are more likely to develop epilepsy. The true effects won't be known unless clinical trials are done on humans and those could result in other findings. A classic example is thalidomide, an anti-morning sickness drug which had the devastating side-effects of causing congenital deformities of the limbs in humans, though no such side-effect had shown up in animals. The results of the older studies were not particularly impressive because they required such high doses that side-effects resulted, Corcoran said. However, the view persisted that marijuana has potential as an anti-epileptic agent that could be used in therapy. Although research on the subject died out, some epileptics who cannot tolerate the normal anticonvulsant drugs use marijuana to control seizures with no previously identified side-effects. While Corcoran is not prepared to dismiss the possibility that marijuana may help control epilepsy, it is also possible users are experiencing a placebo effect, he said. "Our species is remarkably adept at kidding ourselves," he said. - --- MAP posted-by: Larry Seguin