The GABAA Receptor as Target for Novel Heterocyclic Compounds

Nilsson, Jakob

The GABAA Receptor as Target for Novel Heterocyclic Compounds

Mark

Nilsson, Jakob ^LU (2008)

Abstract: Ligands for the benzodiazepine-binding site of the GABAA receptor can belong to structurally diverse classes of compounds including, in spite of the name of the binding site, many non-benzodiazepine structures. The GABAA receptor is a ligand-gated ion channel assembled of five subunits from eight different classes with multiple isoforms. The physiological effect elicited by benzodiazepines is believed to depend particularly on the isoform of the α-subunit. In this study new heterocyclic ligands were designed and synthesized from a pharmacophore model of the benzodiazepine-binding site partly developed in this study. The novel heterocyclic benzodiazepine receptor ligands synthesized include 4-quinolones, aza flavones, triazoloquinazolines,... (More); Ligands for the benzodiazepine-binding site of the GABAA receptor can belong to structurally diverse classes of compounds including, in spite of the name of the binding site, many non-benzodiazepine structures. The GABAA receptor is a ligand-gated ion channel assembled of five subunits from eight different classes with multiple isoforms. The physiological effect elicited by benzodiazepines is believed to depend particularly on the isoform of the α-subunit. In this study new heterocyclic ligands were designed and synthesized from a pharmacophore model of the benzodiazepine-binding site partly developed in this study. The novel heterocyclic benzodiazepine receptor ligands synthesized include 4-quinolones, aza flavones, triazoloquinazolines, isoxazoloquinolones, pyrazoloquinolones, isothiazoloquinolones and isothiazolyl amides. All of these compound classes were active in vitro on the GABAA receptor with the 4-quinolone 72 displaying the highest affinity (Ki = 0.048 nM) so far reported. The 4-quinolones and the aza flavones all displayed selectivity for α1- versus α2- and α3-containing receptors, ranging from 2 to 27. The novel triazoloquinazoline and azoloquinolone scaffolds were designed de novo employing the pharmacophore model. A multigram-synthesis of the triazoloquinazoline 147 was developed and a library of ligands substituted on a position corresponding to the interface region was created. This study demonstrates the high predictive value of the developed benzodiazepine-binding site pharmacophore model and the utilization of de novo design of GABAA ligands. The hypothesis of the novel scaffolds, besides being potent, was they would allow for new substituent patterns in the benzodiazepine-binding site, and guided by molecular modelling, facilitate the development and understanding of GABAA subtype selective ligands. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/1146226

author

Nilsson, Jakob ^LU

supervisor

Olov Sterner ^LU

opponent

Grötli, Morten, Göteborgs Universitet

organization

Centre for Analysis and Synthesis

publishing date

2008

type

Thesis

publication status

published

subject

Organic Chemistry

pages

120 pages

defense location

Sal C, Kemicentrum, Getingev 60, Lund

defense date

2008-05-29 09:30:00

ISBN

978-91-628-7518-3

language

English

LU publication?

yes

additional info

The information about affiliations in this record was updated in December 2015. The record was previously connected to the following departments: Organic chemistry (S/LTH) (011001240)

id

0fc461fd-c1f3-45c2-91bc-8fa1a224ba11 (old id 1146226)

date added to LUP

2016-04-04 14:18:11

date last changed

2018-11-21 21:19:31

@phdthesis{0fc461fd-c1f3-45c2-91bc-8fa1a224ba11,
  abstract     = {{Ligands for the benzodiazepine-binding site of the GABAA receptor can belong to structurally diverse classes of compounds including, in spite of the name of the binding site, many non-benzodiazepine structures. The GABAA receptor is a ligand-gated ion channel assembled of five subunits from eight different classes with multiple isoforms. The physiological effect elicited by benzodiazepines is believed to depend particularly on the isoform of the α-subunit. In this study new heterocyclic ligands were designed and synthesized from a pharmacophore model of the benzodiazepine-binding site partly developed in this study. The novel heterocyclic benzodiazepine receptor ligands synthesized include 4-quinolones, aza flavones, triazoloquinazolines, isoxazoloquinolones, pyrazoloquinolones, isothiazoloquinolones and isothiazolyl amides. All of these compound classes were active in vitro on the GABAA receptor with the 4-quinolone 72 displaying the highest affinity (Ki = 0.048 nM) so far reported. The 4-quinolones and the aza flavones all displayed selectivity for α1- versus α2- and α3-containing receptors, ranging from 2 to 27. The novel triazoloquinazoline and azoloquinolone scaffolds were designed de novo employing the pharmacophore model. A multigram-synthesis of the triazoloquinazoline 147 was developed and a library of ligands substituted on a position corresponding to the interface region was created. This study demonstrates the high predictive value of the developed benzodiazepine-binding site pharmacophore model and the utilization of de novo design of GABAA ligands. The hypothesis of the novel scaffolds, besides being potent, was they would allow for new substituent patterns in the benzodiazepine-binding site, and guided by molecular modelling, facilitate the development and understanding of GABAA subtype selective ligands.}},
  author       = {{Nilsson, Jakob}},
  isbn         = {{978-91-628-7518-3}},
  language     = {{eng}},
  school       = {{Lund University}},
  title        = {{The GABAA Receptor as Target for Novel Heterocyclic Compounds}},
  year         = {{2008}},
}

Lund University Publications

LUND UNIVERSITY LIBRARIES

The GABAA Receptor as Target for Novel Heterocyclic Compounds