Studying the binding interactions of allosteric agonists and antagonists of the CXCR4 receptor

Studying the binding interactions of allosteric agonists and antagonists of the CXCR4 receptor

•Analysis of agonist and antagonist allosteric binding sites in CXCR4.•Agonist pepducin ATI-2341 binds in the intracellular domain of CXCR4.•Antagonists AMD11070 and GSK812397 bind in a subsite in the extracellular pocket. Several examples of allosteric modulators of GPCRs have been reported recentl...

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Veröffentlicht in:Journal of molecular graphics & modelling 2015-07, Vol.60, p.1-14
Hauptverfasser: Planesas, Jesús M., Pérez-Nueno, Violeta I., Borrell, José I., Teixidó, Jordi
Format: Artikel
Sprache:eng
Schlagworte:
Allosteric agonists and antagonists
Allosteric binding sites
Allosteric Regulation
Allosteric Site
Amino Acid Sequence
Aminoquinolines - chemistry
Aminoquinolines - metabolism
Aminoquinolines - pharmacology
Binding
Binding Sites
Blinds
Cellular
CXCR4
Docking
Heterocyclic Compounds, 1-Ring - chemistry
Heterocyclic Compounds, 1-Ring - metabolism
Heterocyclic Compounds, 1-Ring - pharmacology
Humans
Imidazoles - chemistry
Imidazoles - metabolism
Imidazoles - pharmacology
Ligands
Lipopeptides - chemistry
Lipopeptides - metabolism
Lipopeptides - pharmacology
Mathematical models
Models, Molecular
Modulators
Molecular Docking Simulation
Molecular Dynamics Simulation
Molecular Sequence Data
Molecular Structure
Protein Binding
Protein Conformation
Receptors
Receptors, CXCR4 - agonists
Receptors, CXCR4 - antagonists & inhibitors
Receptors, CXCR4 - chemistry
Receptors, CXCR4 - metabolism
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Zusammenfassung:•Analysis of agonist and antagonist allosteric binding sites in CXCR4.•Agonist pepducin ATI-2341 binds in the intracellular domain of CXCR4.•Antagonists AMD11070 and GSK812397 bind in a subsite in the extracellular pocket. Several examples of allosteric modulators of GPCRs have been reported recently in the literature, but understanding their molecular mechanism presents a new challenge for medicinal chemistry. For the specific case of the cellular receptor CXCR4, it is known that pepducins (lipidated fragments of intracellular GPCR loops) such as ATI-2341 modulate CXCR4 activity agonistically via an allosteric mechanism. Moreover, there are also examples of small organic molecules such as AMD11070 and GSK812397 which may also act as allosteric antagonists. However, incomplete knowledge of the ligand-binding sites has hampered a detailed molecular understanding of how these inhibitors work. Here, we attempt to answer this question by analysing the binding interactions between the CXCR4 receptor and the above-mentioned allosteric modulators. We propose two different allosteric binding sites, one located in the intracellular loops 1, 2 and 3 (ICL1, ICL2 and ICL3) which binds the pepducin agonist ATI-2341, and the other at a subsite of the main extracellular orthosteric binding pocket between extracellular loops 1 and 2 and the N-terminus, which binds the antagonists AMD11070 and GSK812397. Allosteric interactions between the CXCR4 and ATI-2341 were predicted by combining different modeling approaches. First, a rotational blind docking search was applied and the best poses were subsequently refined using flexible docking methods and molecular dynamic simulations. For the AMD11070 and GSK812397 antagonists, the entire CXCR4 protein surface was explored by blind docking in order to define the binding region. A second docking analysis by subsites was then performed to refine the allosteric interactions. Finally, we identified the binding residues that appear to be essential for CXCR4 allosteric modulators.
ISSN:1093-3263
1873-4243
DOI:10.1016/j.jmgm.2015.05.004