Allosteric Modulation of GABAA Receptors by an Anilino Enaminone in an Olfactory Center of the Mouse Brain

Allosteric Modulation of GABAA Receptors by an Anilino Enaminone in an Olfactory Center of the Mouse Brain

In an ongoing effort to identify novel drugs that can be used as neurotherapeutic compounds, we have focused on anilino enaminones as potential anticonvulsant agents. Enaminones are organic compounds containing a conjugated system of an amine, an alkene and a ketone. Here, we review the effects of a...

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Main Authors: Thomas Heinbockel, Ze-Jun Wang, Patrice L. Jackson-Ayotunde
Format: Article
Language:English
Published: MDPI AG 2014-12-01
Series:Pharmaceuticals
Subjects:
anticonvulsant
brain slice
enaminone
GABA
GABAA receptor
inhibition
mitral cell
neuromodulation
olfactory bulb
positive allosteric modulator
Online Access:http://www.mdpi.com/1424-8247/7/12/1069
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spelling doaj-b2ff07c4431a4c9b947ec2b3865865362020-11-25T03:18:17ZengMDPI AGPharmaceuticals1424-82472014-12-017121069109010.3390/ph7121069ph7121069Allosteric Modulation of GABAA Receptors by an Anilino Enaminone in an Olfactory Center of the Mouse BrainThomas Heinbockel0Ze-Jun Wang1Patrice L. Jackson-Ayotunde2Department of Anatomy, College of Medicine, Howard University, Washington, DC 20059, USADepartment of Anatomy, College of Medicine, Howard University, Washington, DC 20059, USADepartment of Pharmaceutical Sciences, University of Maryland Eastern Shore, Princess Anne, MD 21853, USAIn an ongoing effort to identify novel drugs that can be used as neurotherapeutic compounds, we have focused on anilino enaminones as potential anticonvulsant agents. Enaminones are organic compounds containing a conjugated system of an amine, an alkene and a ketone. Here, we review the effects of a small library of anilino enaminones on neuronal activity. Our experimental approach employs an olfactory bulb brain slice preparation using whole-cell patch-clamp recording from mitral cells in the main olfactory bulb. The main olfactory bulb is a key integrative center in the olfactory pathway. Mitral cells are the principal output neurons of the main olfactory bulb, receiving olfactory receptor neuron input at their dendrites within glomeruli, and projecting glutamatergic axons through the lateral olfactory tract to the olfactory cortex. The compounds tested are known to be effective in attenuating pentylenetetrazol (PTZ) induced convulsions in rodent models. One compound in particular, KRS-5Me-4-OCF3, evokes potent inhibition of mitral cell activity. Experiments aimed at understanding the cellular mechanism underlying the inhibitory effect revealed that KRS-5Me-4-OCF3 shifts the concentration-response curve for GABA to the left. KRS-5Me-4-OCF3 enhances GABA affinity and acts as a positive allosteric modulator of GABAA receptors. Application of a benzodiazepine site antagonist blocks the effect of KRS-5Me-4-OCF3 indicating that KRS-5Me-4-OCF3 binds at the classical benzodiazepine site to exert its pharmacological action. This anilino enaminone KRS-5Me-4-OCF3 emerges as a candidate for clinical use as an anticonvulsant agent in the battle against epileptic seizures.http://www.mdpi.com/1424-8247/7/12/1069anticonvulsantbrain sliceenaminoneGABAGABAA receptorinhibitionmitral cellneuromodulationolfactory bulbpositive allosteric modulator
collection DOAJ
language English
format Article
sources DOAJ
author Thomas Heinbockel
Ze-Jun Wang
Patrice L. Jackson-Ayotunde
spellingShingle Thomas Heinbockel
Ze-Jun Wang
Patrice L. Jackson-Ayotunde
Allosteric Modulation of GABAA Receptors by an Anilino Enaminone in an Olfactory Center of the Mouse Brain
Pharmaceuticals
anticonvulsant
brain slice
enaminone
GABA
GABAA receptor
inhibition
mitral cell
neuromodulation
olfactory bulb
positive allosteric modulator
author_facet Thomas Heinbockel
Ze-Jun Wang
Patrice L. Jackson-Ayotunde
author_sort Thomas Heinbockel
title Allosteric Modulation of GABAA Receptors by an Anilino Enaminone in an Olfactory Center of the Mouse Brain
title_short Allosteric Modulation of GABAA Receptors by an Anilino Enaminone in an Olfactory Center of the Mouse Brain
title_full Allosteric Modulation of GABAA Receptors by an Anilino Enaminone in an Olfactory Center of the Mouse Brain
title_fullStr Allosteric Modulation of GABAA Receptors by an Anilino Enaminone in an Olfactory Center of the Mouse Brain
title_full_unstemmed Allosteric Modulation of GABAA Receptors by an Anilino Enaminone in an Olfactory Center of the Mouse Brain
title_sort allosteric modulation of gabaa receptors by an anilino enaminone in an olfactory center of the mouse brain
publisher MDPI AG
series Pharmaceuticals
issn 1424-8247
publishDate 2014-12-01
description In an ongoing effort to identify novel drugs that can be used as neurotherapeutic compounds, we have focused on anilino enaminones as potential anticonvulsant agents. Enaminones are organic compounds containing a conjugated system of an amine, an alkene and a ketone. Here, we review the effects of a small library of anilino enaminones on neuronal activity. Our experimental approach employs an olfactory bulb brain slice preparation using whole-cell patch-clamp recording from mitral cells in the main olfactory bulb. The main olfactory bulb is a key integrative center in the olfactory pathway. Mitral cells are the principal output neurons of the main olfactory bulb, receiving olfactory receptor neuron input at their dendrites within glomeruli, and projecting glutamatergic axons through the lateral olfactory tract to the olfactory cortex. The compounds tested are known to be effective in attenuating pentylenetetrazol (PTZ) induced convulsions in rodent models. One compound in particular, KRS-5Me-4-OCF3, evokes potent inhibition of mitral cell activity. Experiments aimed at understanding the cellular mechanism underlying the inhibitory effect revealed that KRS-5Me-4-OCF3 shifts the concentration-response curve for GABA to the left. KRS-5Me-4-OCF3 enhances GABA affinity and acts as a positive allosteric modulator of GABAA receptors. Application of a benzodiazepine site antagonist blocks the effect of KRS-5Me-4-OCF3 indicating that KRS-5Me-4-OCF3 binds at the classical benzodiazepine site to exert its pharmacological action. This anilino enaminone KRS-5Me-4-OCF3 emerges as a candidate for clinical use as an anticonvulsant agent in the battle against epileptic seizures.
topic anticonvulsant
brain slice
enaminone
GABA
GABAA receptor
inhibition
mitral cell
neuromodulation
olfactory bulb
positive allosteric modulator
url http://www.mdpi.com/1424-8247/7/12/1069
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AT zejunwang allostericmodulationofgabaareceptorsbyananilinoenaminoneinanolfactorycenterofthemousebrain
AT patriceljacksonayotunde allostericmodulationofgabaareceptorsbyananilinoenaminoneinanolfactorycenterofthemousebrain
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