Leveraging a Low-Affinity Diazaspiro Orthosteric Fragment to Reduce Dopamine D<sub>3</sub> Receptor (D<sub>3</sub>R) Ligand Promiscuity across Highly Conserved Aminergic G-Protein-Coupled Receptors (GPCRs)

Reilly, Sean W.; Riad, Aladdin; Hsieh, Chia-Ju; Sahlholm, Kristoffer; Jacome, Daniel A.; Griffin, Suzy A.; Taylor, Michelle; Weng, Chi Chang; Xu, Kuiying; Kirschner, Nathan; Luedtke, Robert R.; Parry, C. B. Wynn; Malhotra, Shipra; Karanicolas, John; Mach, Robert H.

doi:10.1021/acs.jmedchem.9b00412

Cited by 17 publications

(12 citation statements)

References 54 publications

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“…To generate SAR, the new library of compounds was tested in radioligand binding assays at both human-cloned D 2 R (hD 2 R) and D 3 R (hD 3 R) receptor subtypes using agonist [ 3 H]-( R )-(+)-7-OH-DPAT and/or antagonist [ 3 H]- N -methylspiperone (Table ). We have found that the D 2 R active state agonist binding is significantly more sensitive ,,, to the radioligand used with respect to D 3 R. As a consequence, the use of [ 3 H]-( R )-(+)-7-OH-DPAT allows an accurate determination of apparent affinities for both targets, and selectivity, valuable to better correlate measured binding values with predicted and/or experimentally determined functional profiles, ,,, which would be otherwise dramatically overestimated in favor of the D 3 R when the antagonist [ 3 H]- N -methylspiperone is used [Table , comparison between D 3 R and D 2 R selectivity ratios between K i s obtained using [ 3 H]- N -methylspiperone or [ 3 H]-( R )-(+)-7-OH-DPAT].…”

Section: Results and Discussionmentioning

confidence: 99%

Chiral Cyclic Aliphatic Linkers as Building Blocks for Selective Dopamine D₂ or D₃ Receptor Agonists

et al. 2021

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Linkers are emerging as a key component in regulating the pharmacology of bitopic ligands directed toward G-protein coupled receptors (GPCRs). In this study, the role of regio- and stereochemistry in cyclic aliphatic linkers tethering well-characterized primary and secondary pharmacophores targeting dopamine D2 and D3 receptor subtypes (D2R and D3R, respectively) is described. We introduce several potent and selective D2R ( rel-trans-16b; D2R K i = 4.58 nM) and D3R ( rel-cis-14a; D3R K i = 5.72 nM) agonists while modulating subtype selectivity in a stereospecific fashion, transferring D2R selectivity toward D3R via inversion of the stereochemistry around these cyclic aliphatic linkers [e.g., (−)-(1S,2R)-43 and (+)-(1R,2S)-42]. Pharmacological observations were supported with extensive molecular docking studies. Thus, not only is it an innovative approach to modulate the pharmacology of dopaminergic ligands described, but a new class of optically active cyclic linkers are also introduced, which can be used to expand the bitopic drug design approach toward other GPCRs.

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Section: Results and Discussionmentioning

confidence: 99%

Chiral Cyclic Aliphatic Linkers as Building Blocks for Selective Dopamine D₂ or D₃ Receptor Agonists

et al. 2021

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“…The molecular docking studies were performed using the previously reported methods [21]. Fallypride, FTP, and KX-02-065 structures were drawn using the ChemDraw Professional 15.1 (PerkinElmer Informatics, Inc., Waltham, MA, USA).…”

Section: Molecular Dockingmentioning

confidence: 99%

Interaction of Ligands for PET with the Dopamine D3 Receptor: In Silico and In Vitro Methods

et al. 2021

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[18F]Fallypride and [18F]Fluortriopride (FTP) are two different PET radiotracers that bind with sub-nanomolar affinity to the dopamine D3 receptor (D3R). In spite of their similar D3 affinities, the two PET ligands display very different properties for labeling the D3R in vivo: [18F]Fallypride is capable of binding to D3R under “baseline” conditions, whereas [18F]FTP requires the depletion of synaptic dopamine in order to image the receptor in vivo. These data suggest that [18F]Fallypride is able to compete with synaptic dopamine for binding to the D3R, whereas [18F]FTP is not. The goal of this study was to conduct a series of docking and molecular dynamic simulation studies to identify differences in the ability of each molecule to interact with the D3R that could explain these differences with respect to competition with synaptic dopamine. Competition studies measuring the ability of each ligand to compete with dopamine in the β-arrestin assay were also conducted. The results of the in silico studies indicate that FTP has a weaker interaction with the orthosteric binding site of the D3R versus that of Fallypride. The results of the in silico studies were also consistent with the IC50 values of each compound in the dopamine β-arrestin competition assays. The results of this study indicate that in silico methods may be able to predict the ability of a small molecule to compete with synaptic dopamine for binding to the D3R.

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“…The dataset of inactives ( SC60 – SC127 ) was also derived from the ChEMBL and comprised 68 compounds with a K I higher than 50 µM. The inactive dataset is shown in Table S2 [ 71 , 72 , 73 , 74 , 75 , 76 , 77 , 78 , 79 , 80 , 81 , 82 , 83 , 84 , 85 , 86 , 87 , 88 , 89 , 90 , 91 , 92 ]. The decoy dataset including 3752 compounds was generated utilizing the DUD-E webtool ( [ 93 ], accessed on 15 March 2021) and based on the structures of the active dataset.…”

Section: Resultsmentioning

confidence: 99%

Identification of Novel Dopamine D2 Receptor Ligands—A Combined In Silico/In Vitro Approach

et al. 2022

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Diseases of the central nervous system are an alarming global problem showing an increasing prevalence. Dopamine receptor D2 (D2R) has been shown to be involved in central nervous system diseases. While different D2R-targeting drugs have been approved by the FDA, they all suffer from major drawbacks due to promiscuous receptor activity leading to adverse effects. Increasing the number of potential D2R-targeting drug candidates bears the possibility of discovering molecules with less severe side-effect profiles. In dire need of novel D2R ligands for drug development, combined in silico/in vitro approaches have been shown to be efficient strategies. In this study, in silico pharmacophore models were generated utilizing both ligand- and structure-based approaches. Subsequently, different databases were screened for novel D2R ligands. Selected virtual hits were investigated in vitro, quantifying their binding affinity towards D2R. This workflow successfully identified six novel D2R ligands exerting micro- to nanomolar (most active compound KI = 4.1 nM) activities. Thus, the four pharmacophore models showed prospective true-positive hit rates in between 4.5% and 12%. The developed workflow and identified ligands could aid in developing novel drug candidates for D2R-associated pathologies.

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Leveraging a Low-Affinity Diazaspiro Orthosteric Fragment to Reduce Dopamine D₃ Receptor (D₃R) Ligand Promiscuity across Highly Conserved Aminergic G-Protein-Coupled Receptors (GPCRs)

Cited by 17 publications

References 54 publications

Chiral Cyclic Aliphatic Linkers as Building Blocks for Selective Dopamine D₂ or D₃ Receptor Agonists

Chiral Cyclic Aliphatic Linkers as Building Blocks for Selective Dopamine D₂ or D₃ Receptor Agonists

Interaction of Ligands for PET with the Dopamine D3 Receptor: In Silico and In Vitro Methods

Identification of Novel Dopamine D2 Receptor Ligands—A Combined In Silico/In Vitro Approach

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Leveraging a Low-Affinity Diazaspiro Orthosteric Fragment to Reduce Dopamine D3 Receptor (D3R) Ligand Promiscuity across Highly Conserved Aminergic G-Protein-Coupled Receptors (GPCRs)

Cited by 17 publications

References 54 publications

Chiral Cyclic Aliphatic Linkers as Building Blocks for Selective Dopamine D2 or D3 Receptor Agonists

Chiral Cyclic Aliphatic Linkers as Building Blocks for Selective Dopamine D2 or D3 Receptor Agonists

Interaction of Ligands for PET with the Dopamine D3 Receptor: In Silico and In Vitro Methods

Identification of Novel Dopamine D2 Receptor Ligands—A Combined In Silico/In Vitro Approach

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Leveraging a Low-Affinity Diazaspiro Orthosteric Fragment to Reduce Dopamine D₃ Receptor (D₃R) Ligand Promiscuity across Highly Conserved Aminergic G-Protein-Coupled Receptors (GPCRs)

Chiral Cyclic Aliphatic Linkers as Building Blocks for Selective Dopamine D₂ or D₃ Receptor Agonists

Chiral Cyclic Aliphatic Linkers as Building Blocks for Selective Dopamine D₂ or D₃ Receptor Agonists