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US: Marijuana-like chemicals bring hope to epileptics

DrugResearcher.com

Friday 17 Sep 2004

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New research in the US, focusing on the pharmacological aspects of smoking
marijuana, are closer to understanding how the drugs active ingredients
exert its effects, paving the way for drugs that selectively bind and block
subtypes of cannabinoid receptors on one type of cell but not another.

The research holds promise as it implies there may be one way to harness
the medically useful aspect of marijuana without causing the associated
brain-altering side effects.

Such research could produce drugs that could be useful in treating
epilepsy. A drug that blocks cannabinoid receptors on some types of
inhibitory interneurons might allow them to continue quieting the
seizure-inducing pyramidal cells during periods of intense activity.

In previous work, other researchers had found that pyramidal cells
manufacture and release cannabinoids that bind to a receptor on the
membrane of interneurons.

The cortex contains two major types of nerve cells. Pyramidal neurons that
excite both local and more distant neighbours, and inhibitory interneurons
that act as local dimming switches, shutting down the activity of nearby
brain cells. The inhibitory interneurons prevent the brain from taking in
and responding to every thought, sight or sound it encounters. They also
protect against runaway excitation such as that seen in epilepsy.

Scientists at Stanford University School of Medicine discovered the drug's
active ingredients tetrahydrocannabinol and related compounds, called
cannabinoids inhibit the group of interneurons that act as information
gatekeepers in the brain's major information processing centre, called the
cerebral cortex.

These interneurons also release cannabinoids that quiet their own activity.
This form of self-inhibition is a novel way for neurons to regulate their
own ability to send messages to their neighbours. Tetrahydrocannabinol from
marijuana may work its brain-altering magic by binding to these same cells.

The research headed up by David Prince and Irene Thiele Pimley, Professor
of Neurology and Neurological Sciences is published in the Sept. 16 issue
of Nature.

The class of interneurons, the "LTS cells" of the cerebral cortex,
manufacture and release cannabinoids that bind to their own cannabinoid
receptors and shut down their ability to signal other neurons. By shutting
themselves off, the interneurons block their quieting action on the
excitatory pyramidal cells. Without the quieting effect, pyramidal cells
signal more intensely, triggering a higher level of activity in circuits of
the cortex.

Prince commented: "A loss of inhibition in pyramidal cells could produce
changes in perception, in motor function and in everything the cerebral
cortex does."

During an epileptic seizure, Pyramidal cells are among those that fire out
of control during a seizure. One reason these cells fire so rapidly may be
that interneurons get shut down.

With 300,000 people in the UK suffering from epilepsy (40 million people
worldwide), the need for specialised but effective anti-epileptic drugs
(AED) has never been more called for.

The identification of SV2A as the binding site for AED Keppra provides an
innovative and unique drug discovery platform to identify new drugs with
improved characteristics. It also provides molecular evidence that Keppra
is different from all other anti-epileptic and CNS drugs. No other known
anti-epileptic drugs (AED's) bind to SV2A.


 

 

 

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