In vitro and in vivo characterization of MPEP,an allosteric modulator of the metabotropic glutamate receptor subtype 5: review article |
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Authors: | Kuhn R Pagano A Stoehr N Vranesic I Flor P J Lingenhöhl K Spooren W Gentsch C Vassout A Pilc A Gasparini F |
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Affiliation: | (1) Nervous System Research, Novartis, Pharma AG, Basel, Switzerland, CH;(2) Institute of Pharmacology, Polish Academy of Science, Krakow, Poland, PL |
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Abstract: | Summary. There is a need to identify subtype-specific ligands for mGlu receptors to elucidate the potential of these receptors for
the treatment of nervous system disorders. To date, most mGlu receptor antagonists are amino acid-like compounds acting as
competitive antagonists at the glutamate binding site located in the large extracellular N-terminal domain.
We have characterized novel subtype-selective mGlu5 receptor antagonists which are structurally unrelated to competitive mGlu receptor ligands. Using a series of chimeric receptors
and point mutations we demonstrate that these antagonists act as inverse agonists with a novel allosteric binding site in
the seven-transmembrane domain. Recent studies in animal models implicate mGlu5 receptors as a potentially important therapeutic target particularly for the treatment of pain and anxiety.
Received July 2, 2001 Accepted August 6, 2001 Published online September 10, 2002 |
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Keywords: | : Group I metabotropic glutamate receptors MPEP SIB-1757 Anxiety Pain |
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