Abstract

The overall goal of this proposed interdisciplinary effort continues to be the computer assisted design of new therapeutic agents with improved pharmacological profiles, which exert their effects by binding to the BDZ/GABA-A receptor (BDZR ligands). To this end, we shall continue to 1) validate current hypotheses for non selective ligands involving common molecular determinants of recognition of BDZ/GABA-A receptor(s) and determinants of activation based on their anticonvulsant endpoint and identify promising medications designed using them. This goal will be accomplished by: a) Continued theoretical characterization of additional families of compounds reported in the literature that were not included in the original data set for hypothesis development, and b) synthesis and pharmacological evaluation of two of the families with predicted pharmacological profiles originally proposed based on this hypothesis: i) azaindoles; ii) pyrroloquinolines. 2) Enhance knowledge of BDZ in vitro and in vivo pharmacology in light of emerging developments in molecular biology, in a manner that will also result in an appropriate database for hypothesis refinement and design of second generation analogs. To accomplish this aim we shall: a) Synthesize analogs of compounds that have been reported to have interesting pharmacological profiles that could be useful to i) probe receptor heterogeneity because of their ability to bind selectively or ii) elicit qualitatively different responses i.e. agonism, antagonism, inverse agonism or no response in different behavioral endpoints, b) Continue to characterize receptor heterogeneity, addressing the question of the number of central BDZR subtypes using different brain regions reported to have limited subtype heterogeneity and using additional ligands; c) Explore the usefulness of chloride ion flux as an indication of agonist, antagonist and inverse agonist activity in each brain region used for receptor binding studies; d) Use the six in vivo endpoints: anxiolytic, anticonvulsant, hyperphagia, sedation, muscle relaxant and hypothermia, to characterize additional known families and the newly synthesized ones, found to bind with significant affinity to any BDZ/GABA-A receptor subtype. The goal of these studies is to determine promising differences in the ability of a set of chosen compounds to differentially elicit these activities. These results will be useful for two different purposes: i) to serve as a database for the design of activity-specific analogs and ii) to further elucidate the relationship between recognition of a given subtype and in vivo responses. 3.Use the techniques of theoretical chemistry for the same compounds to be studied experimentally, in an """"""""interim"""""""" design strategy based on molecular determinants of activation at each in vivo endpoint. Implicit in this approach is the determination of common properties modulating recognition of all receptors involved in the particular endpoint considered. This strategy will lead to refinements of our current hypotheses that will be used to design activity-selective compounds that could be more targeted medications.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Research Project (R01)
Project #
5R01DA006304-05
Application #
2118623
Study Section
Drug Abuse Biomedical Research Review Committee (DABR)
Program Officer
Hillery, Paul
Project Start
1989-09-30
Project End
1995-08-31
Budget Start
1993-09-01
Budget End
1994-08-31
Support Year
5
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
Molecular Research Institute
Department
Type
DUNS #
017430633
City
Palo Alto
State
CA
Country
United States
Zip Code
94303

  Publications

Wisor, Jonathan P; DeLorey, Timothy M; Homanics, Gregg E et al. (2002) Sleep states and sleep electroencephalographic spectral power in mice lacking the beta 3 subunit of the GABA(A) receptor. Brain Res 955:221-8
Lameh, J; Keohane, A; Clark, D J et al. (2001) Characterization of novel benzodiazepine ligands in Spodotera frugiperda (Sf-9) insect cells. Neurosci Lett 306:25-8
DeLorey, T M; Lin, R C; McBrady, B et al. (2001) Influence of benzodiazepine binding site ligands on fear-conditioned contextual memory. Eur J Pharmacol 426:45-54
Filizola, M; Harris, D L; Loew, G H (2000) Benzodiazepine-induced hyperphagia: development and assessment of a 3D pharmacophore by computational methods. J Biomol Struct Dyn 17:769-78
Lameh, J; Wang, P; Meredith, D et al. (2000) Characterization of benzodiazepine receptors in the cerebellum. Prog Neuropsychopharmacol Biol Psychiatry 24:979-91
Harris, D L; Loew, G (2000) Development and assessment of a 3D pharmacophore for ligand recognition of BDZR/GABAA receptors initiating the anxiolytic response. Bioorg Med Chem 8:2527-38
Filizola, M; Harris, D L; Loew, G H (2000) Development of a 3D pharmacophore for nonspecific ligand recognition of alpha1, alpha2, alpha3, alpha5, and alpha6 containing GABA(A)/benzodiazepine receptors. Bioorg Med Chem 8:1799-807
Lameh, J; Wang, P; Elgart, D et al. (2000) Unraveling the identity of benzodiazepine binding sites in rat hipppocampus and olfactory bulb. Eur J Pharmacol 400:167-76
Harris, D L; DeLorey, T M; He, X et al. (2000) Determinants of recognition of ligands binding to benzodiazepine receptor/GABA(A) receptors initiating sedation. Eur J Pharmacol 401:271-87
Chen, S W; Chen, H A; Davies, M F et al. (1996) Putative benzodiazepine partial agonists demonstrate receptor heterogeneity. Pharmacol Biochem Behav 53:87-97

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