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Structure–activity studies of 3,9-diazaspiro[5.5]undecane-based γ-aminobutyric acid type A receptor antagonists with immunomodulatory effect

Structure–activity studies of 3,9-diazaspiro[5.5]undecane-based γ-aminobutyric acid type A receptor antagonists with immunomodulatory effect
Structure–activity studies of 3,9-diazaspiro[5.5]undecane-based γ-aminobutyric acid type A receptor antagonists with immunomodulatory effect
The 3,9-diazaspiro[5.5]undecane-based compounds 2027 and 018 have previously been reported to be potent competitive γ-aminobutyric acid type A receptor (GABAAR) antagonists showing low cellular membrane permeability. Given the emerging peripheral application of GABAAR ligands, we hypothesize 2027 analogs as promising lead structures for peripheral GABAAR inhibition. We herein report a study on the structural determinants of 2027 in order to suggest a potential binding mode as a basis for rational design. The study identified the importance of the spirocyclic benzamide, compensating for the conventional acidic moiety, for GABAAR ligands. The structurally simplified m-methylphenyl analog 1e displayed binding affinity in the high-nanomolar range (Ki = 180 nM) and was superior to 2027 and 018 regarding selectivity for the extrasynaptic α4βδ subtype versus the α1- and α2- containing subtypes. Importantly, 1e was shown to efficiently rescue inhibition of T cell proliferation, providing a platform to explore the immunomodulatory potential for this class of compounds.
0022-2623
17795-17812
Bavo, Francesco
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De-jong, Heleen
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Petersen, Jonas
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Falk-petersen, Christina Birkedahl
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Löffler, Rebekka
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Sparrow, Emma
36c640a3-bda9-4332-a3b5-99ff9d803e5b
Rostrup, Frederik
558148b7-0494-4e0e-bc74-02269c6cbadf
Eliasen, Jannik Nicklas
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Wilhelmsen, Kristine S.
1b0bfe99-6261-428e-bd28-42050226166d
Barslund, Kasper
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Bundgaard, Christoffer
c91d70db-15d8-4ce5-9578-3c535cb7cf42
Nielsen, Birgitte
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Kristiansen, Uffe
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Wellendorph, Petrine
2902b8b3-7fcc-42e6-ac21-7a7c09b990be
Bogdanov, Yury
0c970999-e191-4f1b-90d9-7bf25a5d5b4b
Frølund, Bente
c2eb6c7e-b23e-48e1-b679-20094ea32f38
Bavo, Francesco
e3fe6a1f-08a1-46f2-827d-fdd1afc0acfc
De-jong, Heleen
1bedc37e-b88b-477f-b5bd-a47179008865
Petersen, Jonas
d9f61a92-0294-453a-9f76-1dc51aa304cf
Falk-petersen, Christina Birkedahl
a3418759-059a-48d3-bf67-eb59e52ebd7a
Löffler, Rebekka
29cb75ff-a668-4b98-a230-09bbf954bba4
Sparrow, Emma
36c640a3-bda9-4332-a3b5-99ff9d803e5b
Rostrup, Frederik
558148b7-0494-4e0e-bc74-02269c6cbadf
Eliasen, Jannik Nicklas
5b09d5e7-b998-44d0-a01b-699d9e324735
Wilhelmsen, Kristine S.
1b0bfe99-6261-428e-bd28-42050226166d
Barslund, Kasper
12c3e59b-cf49-4b32-9701-327bc36aee73
Bundgaard, Christoffer
c91d70db-15d8-4ce5-9578-3c535cb7cf42
Nielsen, Birgitte
5e865b96-5b4c-4cc1-bc90-a03f41769c1a
Kristiansen, Uffe
846f2cef-b8bb-4ebf-93b9-5f47f67b98bc
Wellendorph, Petrine
2902b8b3-7fcc-42e6-ac21-7a7c09b990be
Bogdanov, Yury
0c970999-e191-4f1b-90d9-7bf25a5d5b4b
Frølund, Bente
c2eb6c7e-b23e-48e1-b679-20094ea32f38

Bavo, Francesco, De-jong, Heleen, Petersen, Jonas, Falk-petersen, Christina Birkedahl, Löffler, Rebekka, Sparrow, Emma, Rostrup, Frederik, Eliasen, Jannik Nicklas, Wilhelmsen, Kristine S., Barslund, Kasper, Bundgaard, Christoffer, Nielsen, Birgitte, Kristiansen, Uffe, Wellendorph, Petrine, Bogdanov, Yury and Frølund, Bente (2021) Structure–activity studies of 3,9-diazaspiro[5.5]undecane-based γ-aminobutyric acid type A receptor antagonists with immunomodulatory effect. Journal of Medicinal Chemistry, 64 (24), 17795-17812. (doi:10.1021/acs.jmedchem.1c00290).

Record type: Article

Abstract

The 3,9-diazaspiro[5.5]undecane-based compounds 2027 and 018 have previously been reported to be potent competitive γ-aminobutyric acid type A receptor (GABAAR) antagonists showing low cellular membrane permeability. Given the emerging peripheral application of GABAAR ligands, we hypothesize 2027 analogs as promising lead structures for peripheral GABAAR inhibition. We herein report a study on the structural determinants of 2027 in order to suggest a potential binding mode as a basis for rational design. The study identified the importance of the spirocyclic benzamide, compensating for the conventional acidic moiety, for GABAAR ligands. The structurally simplified m-methylphenyl analog 1e displayed binding affinity in the high-nanomolar range (Ki = 180 nM) and was superior to 2027 and 018 regarding selectivity for the extrasynaptic α4βδ subtype versus the α1- and α2- containing subtypes. Importantly, 1e was shown to efficiently rescue inhibition of T cell proliferation, providing a platform to explore the immunomodulatory potential for this class of compounds.

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Accepted/In Press date: 15 December 2021
e-pub ahead of print date: 15 December 2021
Published date: 23 December 2021

Identifiers

Local EPrints ID: 454543
URI: http://eprints.soton.ac.uk/id/eprint/454543
ISSN: 0022-2623
PURE UUID: 9e571082-94d0-4de2-8193-8bb526687919
ORCID for Yury Bogdanov: ORCID iD orcid.org/0000-0003-4667-5890

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Date deposited: 15 Feb 2022 17:43
Last modified: 17 Mar 2024 07:07

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Contributors

Author: Francesco Bavo
Author: Heleen De-jong
Author: Jonas Petersen
Author: Christina Birkedahl Falk-petersen
Author: Rebekka Löffler
Author: Emma Sparrow
Author: Frederik Rostrup
Author: Jannik Nicklas Eliasen
Author: Kristine S. Wilhelmsen
Author: Kasper Barslund
Author: Christoffer Bundgaard
Author: Birgitte Nielsen
Author: Uffe Kristiansen
Author: Petrine Wellendorph
Author: Yury Bogdanov ORCID iD
Author: Bente Frølund

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