Exploring the molecular determinants for subtype-selectivity of 2-amino-1,4,5,6-tetrahydropyrimidine-5-carboxylic acid analogs as betaine/GABA transporter 1 (BGT1) substrate-inhibitors

Kickinger, Stefanie; Al-Khawaja, Anas; Haugaard, Anne S.; Lie, Maria E. K.; Bavo, Francesco; Löffler, Rebekka; Damgaard, Maria; Ecker, Gerhard F.; Frølund, Bente; Wellendorph, Petrine

doi:10.1038/s41598-020-69908-w

Cited by 7 publications

(15 citation statements)

References 64 publications

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“…The increase is especially remarkable for bicyclo-GABA approaching a potency of 40 nM. This finding is in line with previous findings, making this a consistent phenomenon among different compound classes ( Kickinger et al, 2020 ). Even though we do not understand the underlying nature of this phenomenon, we speculate that it could be related to the size of the residue (bulky glutamine/tyrosine versus small alanine).…”

Section: Discussionsupporting

confidence: 92%

“…Even though we do not understand the underlying nature of this phenomenon, we speculate that it could be related to the size of the residue (bulky glutamine/tyrosine versus small alanine). However, previous MD simulations of the E52A mutant bound to the GABA analog ATPCA did not reveal additional insights into this ( Kickinger et al, 2020 ). Most likely the used homology model does not provide the necessary accuracy to draw such conclusions.…”

Section: Discussionmentioning

confidence: 93%

“…This assay detects changes in membrane potential for an average cell population through changes in fluorescence of a membrane pre-equilibrated fluorescent blue dye. It therefore provides an indirect measure of activity with the advantage of being able to discern between GAT substrates and inhibitors ( Kragholm et al, 2013 ; Al-Khawaja et al, 2014 ; Kickinger et al, 2020 ).…”

Section: Resultsmentioning

confidence: 99%

“…Furthermore, we wanted to test the double mutant E52Y + Q299L. However, in a previous study this mutant was proven non-functional ( Kickinger et al, 2020 ). Instead, we generated the double mutant E52A + Q299L as well as the single mutant E52A.…”

Section: Resultsmentioning

confidence: 99%

“…This could be due to the fact that 2 can undergo one hydrogen bond less than bicyclo-GABA, which can also explain why 2 is less subtype selective and shows some GAT3 activity ( Table 2 ). In a previous study, we have already identified Q299 and E52 in BGT1 as part of the molecular determinants driving activity and selectivity of a series of cyclic 2-amino-tetrahydropyrimidine/pyridine compounds ( Kickinger et al, 2020 ). We therefore conclude that the interaction between the amino moiety of different BGT1 compound classes with Q299 and E52 is a general key feature for selective BGT1 inhibition ( Jørgensen et al, 2017 ; Kickinger et al, 2020 ; Lie et al, 2020 ).…”

Section: Discussionmentioning

confidence: 99%

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Molecular Determinants and Pharmacological Analysis for a Class of Competitive Non-transported Bicyclic Inhibitors of the Betaine/GABA Transporter BGT1

et al. 2021

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The betaine/GABA transporter 1 (BGT1) is a member of the GABA transporter (GAT) family with still elusive function, largely due to a lack of potent and selective tool compounds. Based on modeling, we here present the design, synthesis and pharmacological evaluation of five novel conformationally restricted cyclic GABA analogs related to the previously reported highly potent and selective BGT1 inhibitor (1S,2S,5R)-5-aminobicyclo[3.1.0]hexane-2-carboxylic acid (bicyclo-GABA). Using [3H]GABA radioligand uptake assays at the four human GATs recombinantly expressed in mammalian cell lines, we identified bicyclo-GABA and its N-methylated analog (2) as the most potent and selective BGT1 inhibitors. Additional pharmacological characterization in a fluorescence-based membrane potential assay showed that bicyclo-GABA and 2 are competitive inhibitors, not substrates, at BGT1, which was validated by a Schild analysis for bicyclo-GABA (pKB value of 6.4). To further elaborate on the selectivity profile both compounds were tested at recombinant α1β2γ2 GABAA receptors. Whereas bicyclo-GABA showed low micromolar agonistic activity, the N-methylated 2 was completely devoid of activity at GABAA receptors. To further reveal the binding mode of bicyclo-GABA and 2 binding hypotheses of the compounds were obtained from in silico-guided mutagenesis studies followed by pharmacological evaluation at selected BGT1 mutants. This identified the non-conserved BGT1 residues Q299 and E52 as the molecular determinants driving BGT1 activity and selectivity. The binding mode of bicyclo-GABA was further validated by the introduction of activity into the corresponding GAT3 mutant L314Q (38 times potency increase cf. wildtype). Altogether, our data reveal the molecular determinants for the activity of bicyclic GABA analogs, that despite their small size act as competitive inhibitors of BGT1. These compounds may serve as valuable tools to selectively and potently target BGT1 in order to decipher its elusive pharmacological role in the brain and periphery such as the liver and kidneys.

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Section: Discussionsupporting

confidence: 92%

Section: Discussionmentioning

confidence: 93%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Molecular Determinants and Pharmacological Analysis for a Class of Competitive Non-transported Bicyclic Inhibitors of the Betaine/GABA Transporter BGT1

et al. 2021

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Structural and stereochemical determinants for hGAT3 inhibition: development of novel conformationally constrained and substituted analogs of (S)-isoserine

Bavo,

Kickinger,

Lie

et al. 2023

Med Chem Res

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The GABA transporter 3 (GAT3) is a member of the GABA transporter (GAT) family proposed to have a role in regulating tonic inhibition. The GAT3-preferring substrate (S)-isoserine has shown beneficial effects in a mouse model of stroke accompanied by an increased GAT3 expression, indicating a molecular mechanism mediated by GAT3. However, (S)-isoserine is not ideally suited for in vivo studies due to a lack of selectivity and brain permeability. To elucidate the structural determinants of (S)-isoserine for GAT3 inhibition, and to optimize and inform further ligand development, we here present the design, synthesis and pharmacological evaluation of a series of conformationally constrained isoserine analogs with defined stereochemistry. Using [3H]GABA uptake assays at recombinant human GAT3, we identified the azetidine and pyrrolidine analogs (2S,2´S)-6 and (2S,2´S)-7 as the most potent inhibitors. To further elaborate on the selectivity profile both compounds were tested at all GATs, the taurine transporter (TauT) and GABAA receptors. Although (2S,2´S)-6 and (2S,2´S)-7 are comparable to (S)-isoserine with respect to potency, the selectivity vs. the taurine transporter was significantly improved (at least 6 and 53 times more activity at hGAT3, respectively). A subsequent comprehensive structure-activity study showed that different connectivity approaches, stereochemical variations, simple or larger α- and N-substituents, and even minor size enlargement of the heterocyclic ring all abrogated GAT3 inhibition, indicating very strict stereochemical and size requirements. The observed structure activity relationships may guide future ligand optimization and the novel ligands ((2S,2´S)-6 and (2S,2´S)-7) can serve as valuable tools to validate the proposed GAT3-mediated effect of (S)-isoserine such as in functional recovery after stroke and thus help corroborate the relevance of targeting GAT3 and tonic inhibition in relevant brain pathologies.

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Development of tricyclic N-benzyl-4-hydroxybutanamide derivatives as inhibitors of GABA transporters mGAT1-4 with anticonvulsant, antinociceptive, and antidepressant activity

Zaręba

Sałat

Höfner

et al. 2021

European Journal of Medicinal Chemistry

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Exploring the molecular determinants for subtype-selectivity of 2-amino-1,4,5,6-tetrahydropyrimidine-5-carboxylic acid analogs as betaine/GABA transporter 1 (BGT1) substrate-inhibitors

Cited by 7 publications

References 64 publications

Molecular Determinants and Pharmacological Analysis for a Class of Competitive Non-transported Bicyclic Inhibitors of the Betaine/GABA Transporter BGT1

Molecular Determinants and Pharmacological Analysis for a Class of Competitive Non-transported Bicyclic Inhibitors of the Betaine/GABA Transporter BGT1

Structural and stereochemical determinants for hGAT3 inhibition: development of novel conformationally constrained and substituted analogs of (S)-isoserine

Development of tricyclic N-benzyl-4-hydroxybutanamide derivatives as inhibitors of GABA transporters mGAT1-4 with anticonvulsant, antinociceptive, and antidepressant activity

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