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From Pyrroles to 1-oxo-2,3,4,9-tetrahydro-1H-beta-carbolines: a New Class of Orally Bioavailable MGluR1 Antagonists

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Specialty Biochemistry
Date 2007 Feb 6
PMID 17276684
Citations 11
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Abstract

Exploiting the SAR of the known pyrrole derivatives, a new class of mGluR1 antagonists was designed by replacement of the pyrrole core with an indole scaffold and consequent cyclization of the C-2 position into a tricyclic beta-carboline template. The appropriate exploration of the position C-6 with a combination of H-bond acceptor groups coupled with bulky/lipophilic moieties led to the discovery of a new series of mGluR1 antagonists. These compounds exhibited a non-competitive behavior, excellent pharmacokinetic properties, and good in vivo activity in animal models of acute and chronic pain, after oral administration.

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