A structural chemogenomics analysis of aminergic <scp>GPCRs</scp>: lessons for histamine receptor ligand design

Kooistra, Albert J.; Kuhne, Sebastiaan; Esch, Iwan J. P. de; Leurs, Rob; Graaf, Chris de

doi:10.1111/bph.12248

Cited by 80 publications

(100 citation statements)

References 175 publications

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“…Yet, the H 2 receptor possesses many of the key prototypical amino acid residues common to the family A aminergic GPCRs, and homology modeling on the basis of the published H 1 receptor X-ray structure and available mutagenesis data leads to reasonable models (Fig. 2) for the interaction of histamine with the receptor protein Histamine Receptors (Kooistra et al, 2013 ). Mutation of either-alone or simultaneously-did not abolish histamine-induced cAMP but markedly reduced its efficacy.…”

Section: A Receptor Structurementioning

confidence: 99%

“…Like for all biogenic amine receptors, the H 3 receptor contains the conserved Asp residue in TM3 (Asp114 3.32 ), which is suggested to be involved in the binding of the ethylamine side chain of histamine ( Fig. 2) (Kooistra et al, 2013 , this might also explain the substantially higher affinity of histamine for H 3 receptors (and also H 4 receptors; see Fig. 3; Tables 1 and 2) (Kooistra et al, 2013).…”

Section: A Receptor Structurementioning

confidence: 99%

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International Union of Basic and Clinical Pharmacology. XCVIII. Histamine Receptors

et al. 2015

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Section: A Receptor Structurementioning

confidence: 99%

Section: A Receptor Structurementioning

confidence: 99%

International Union of Basic and Clinical Pharmacology. XCVIII. Histamine Receptors

et al. 2015

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“…All aminergic GPCRs and some other rhodopsin-like GPCRs, e.g., opioid receptors, share the negatively charged and conserved aspartate residue (D3.32) in the transmembrane helix 3 (TM3) which was generally proposed as a key anchor for the basic moieties of aminergic ligands (Shi and Javitch 2002;Surgand et al 2006;Kooistra et al 2013). Accordingly, most dopamine D 2 receptor orthosteric ligands, including both agonists and antagonists fulfill the criteria of the classical pharmacophore model.…”

Section: Introductionmentioning

confidence: 99%

Synthesis, antibacterial, and antifungal activities of new drimane sesquiterpenoids with azaheterocyclic units

et al. 2016

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The dopaminergic hypothesis of schizophrenia is the main concept explaining the direct reasons of schizophrenia and the effectiveness of current antipsychotics. All antipsychotics present on the market are potent dopamine D 2 receptor antagonists or partial agonists. In this work we investigate a series of dopamine D 2 receptor antagonists which do not fulfill the criteria of the classical pharmacophore model as they do not possess a protonatable nitrogen atom necessary to interact with the conserved Asp(3.32). Such compounds are interesting, inter alia, due to possible better pharmacokinetic profile when compared to basic, ionizable molecules. By means of homology modeling, molecular docking and molecular dynamics we determined that the compounds investigated interact with Asp(3.32) via their amide nitrogen atom. It was found that the studied compounds stabilize the receptor inactive conformation through the effect on the ionic lock, which is typical for GPCR antagonists. We constructed a CoMFA model for the studied compounds with the following statistics:63. The quality of the CoMFA model was confirmed by high value of R 2 of the test set, equal 0.96. The CoMFA model indicated two regions where bulky substituents are favored and two regions where bulky substituents are not beneficial. Two red contour regions near carbonyl groups were identified meaning that negative charge would be favored here. Furthermore, the S-oxide group is connected with blue contour region meaning that positive charge is favored in this position. These findings may be applied for further optimization of the studied compound series.

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“…The combination of molecular pharmacology and structural data provides a powerful lens to gain new insights into the mechanistic details of GPCR function. For instance, a systematic analysis of the functional data available for crystallized ligand-receptor complexes is crucial to elucidate the molecular determinants of ligand binding, including details of structure-activity relationships, which, in turn, can be used to extrapolate the available information to ligands and receptors that are related to known structures but have not yet been crystallized (Kooistra et al, 2013).…”

Section: Complementing Gpcr Structural Chemogenomics With Molecular Pmentioning

confidence: 99%

“…Finally, the cocrystallized doxepin (H 1 R), (R)-3-quinuclidinylbenzilate (muscarinic acetylcholine receptor M 2 [M 2 R]), and tiotropium (M 3 R) ligands share an amine, with two aromatic rings oriented in a butterfly shape (Fig. 5C), with many other H 1 R, M 2 R, and M 3 R ligands (Kooistra et al, 2013).…”

Section: Complementing Gpcr Structural Chemogenomics With Molecular Pmentioning

confidence: 99%

A Molecular Pharmacologist’s Guide to G Protein–Coupled Receptor Crystallography

et al. 2015

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G protein-coupled receptor (GPCR) structural biology has progressed dramatically in the last decade. There are now over 120 GPCR crystal structures deposited in the Protein Data Bank of 32 different receptors from families scattered across the phylogenetic tree, including class B, C, and Frizzled GPCRs. These structures have been obtained in combination with a wide variety of ligands and captured in a range of conformational states. This surge in structural knowledge has enlightened research into the molecular recognition of biologically active molecules, the mechanisms of receptor activation, the dynamics of functional selectivity, and fueled structure-based drug design efforts for GPCRs. Here we summarize the innovations in both protein engineering/molecular biology and crystallography techniques that have led to these advances in GPCR structural biology and discuss how they may influence the resulting structural models. We also provide a brief molecular pharmacologist's guide to GPCR X-ray crystallography, outlining some key aspects in the process of structure determination, with the goal to encourage noncrystallographers to interrogate structures at the molecular level. Finally, we show how chemogenomics approaches can be used to marry the wealth of existing receptor pharmacology data with the expanding repertoire of structures, providing a deeper understanding of the mechanistic details of GPCR function.

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A structural chemogenomics analysis of aminergic GPCRs: lessons for histamine receptor ligand design

Cited by 80 publications

References 175 publications

International Union of Basic and Clinical Pharmacology. XCVIII. Histamine Receptors

International Union of Basic and Clinical Pharmacology. XCVIII. Histamine Receptors

Synthesis, antibacterial, and antifungal activities of new drimane sesquiterpenoids with azaheterocyclic units

A Molecular Pharmacologist’s Guide to G Protein–Coupled Receptor Crystallography

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