Homology modelling of the human adenosine A2B receptor based on X-ray structures of bovine rhodopsin, the β2-adrenergic receptor and the human adenosine A2A receptor

Sherbiny, Farag F.; Schiedel, Anke C.; Maaß, Astrid; Müller, Christian

doi:10.1007/s10822-009-9299-7

Cited by 40 publications

(53 citation statements)

References 63 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Their results have suggested that to best exploit comparative models in molecular docking screens one should use consensus enrichment calculations that include multiple models as well as templates. Others have also addressed issues of docking into homology models (13,(15)(16)(17); for docking into homology models of G-Protein Coupled Receptors (GPCRs), see below.…”

Section: Receptor Representation In Docking Receptor Sourcementioning

confidence: 99%

Challenges and advances in computational docking: 2009 in review

Yuriev

Agostino

Ramsland

2010

J of Molecular Recognition

298

196

View full text Add to dashboard Cite

Docking is a computational technique that places a small molecule (ligand) in the binding site of its macromolecular target (receptor) and estimates its binding affinity. This review addresses methodological developments that have occurred in the docking field in 2009, with a particular focus on the more difficult, and sometimes controversial, aspects of this promising computational discipline. These developments aim to address the main challenges of docking: receptor representation (such aspects as structural waters, side chain protonation, and, most of all, flexibility (from side chain rotation to domain movement)), ligand representation (protonation, tautomerism and stereoisomerism, and the effect of input conformation), as well as accounting for solvation and entropy of binding. This review is strongly focused on docking advances in the context of drug design, specifically in virtual screening and fragment-based drug design.

show abstract

Section: Receptor Representation In Docking Receptor Sourcementioning

confidence: 99%

Challenges and advances in computational docking: 2009 in review

Yuriev

Agostino

Ramsland

2010

J of Molecular Recognition

298

196

View full text Add to dashboard Cite

show abstract

“…The original 3D homology model of the human A 2B AR was based on the inactive, inverse agonist-bound A 2A AR (3EML) [15,16]. After exchange of the EL2 (the A 2B loop was exchanged for the A 2A loop) the model was energy-minimized again and subjected to molecular dynamics simulation as previously described [14].…”

Section: Homology Modelling and Dockingmentioning

confidence: 99%

“…This is particularly true for homology models of closely related receptor subtypes. One example is the A 2B adenosine receptor (A 2B AR) model [14,15], which has been constructed based on X-ray structures of the closely related A 2A AR [16,17].…”

Section: Introductionmentioning

confidence: 99%

The second extracellular loop of GPCRs determines subtype-selectivity and controls efficacy as evidenced by loop exchange study at A2 adenosine receptors

Seibt

Schiedel

Thimm

et al. 2013

Biochemical Pharmacology

Self Cite

View full text Add to dashboard Cite

“…The A 2B receptor encodes a protein of 328 to 332 amino acid residues depending on the species [Pierce et al, 1992]. As a result, a new and improved homology model for the human adenosine A 2B receptor was created and investigated [Sherbiny et al, 2009]. Consequently, virtual screening of potential ligands using the adenosine A 2B receptor model has been accomplished.…”

Section: (Figure 1)schematic Diagram Of a Gpcr With Seven Tm Domains mentioning

confidence: 99%

“…The protein target needs to be prepared and modeled according to the format requirements of the docking algorithms used. Thus the homology model of the human A 2B adenosine receptor [Sherbiny et al, 2009] was used. All bound water ligand were removed from the protein prior to the docking process…”

Section: Molecular Docking Proceduresmentioning

confidence: 99%

Synthesis, Biological Evaluation and Binding Studies of New Flavone Derivatives as Adenosine A2b Receptor Antagonists

Sherbiny

2016

Al-Azhar Journal of Pharmaceutical Sciences

View full text Add to dashboard Cite

A series of eleven flavone derivatives were synthesized. The synthesized compounds were characterized structurally by various techniques using spectral analyses. All of the synthesized compounds were subjected to MTT proliferation assay to investigate their in-vitro cytotoxic activity. Among all the studied compounds, compounds, VIi, VIh, VId and VIk revealed moderate growth inhibitory effect towards the MDA-MB 231 cell line compared to the reference, doxorubicin. These compounds showed cytotoxicity activity with IC 50 values ranging from 43.7 to 138 µM in MDA-MB 231 cell line. The results of cytotoxic activity revealed that flavone derivatives with N-aryl acetamide substituted at the 3-position of flavone backbone have better cytotoxic activity. Moreover, the highest activity was observed with compound VIi that has oxy-N-pyriden-2-yl acetamide substituent at the 3-position of flavone backbone followed by compound VIh with IC 50 values of 43.7 and 50 μM, respectively. The biological activity results were elucidated by molecular docking studies using the homology model of the human adenosine A 2B receptor. As a result, the present study has highlighted that the bicyclic moiety of the compounds attached to hydrogen bond donor-acceptor capability and π-π stacking is an attractive scaffold for obtaining cytotoxic activity.

show abstract

Homology modelling of the human adenosine A2B receptor based on X-ray structures of bovine rhodopsin, the β2-adrenergic receptor and the human adenosine A2A receptor

Cited by 40 publications

References 63 publications

Challenges and advances in computational docking: 2009 in review

Challenges and advances in computational docking: 2009 in review

The second extracellular loop of GPCRs determines subtype-selectivity and controls efficacy as evidenced by loop exchange study at A2 adenosine receptors

Synthesis, Biological Evaluation and Binding Studies of New Flavone Derivatives as Adenosine A2b Receptor Antagonists

Contact Info

Product

Resources

About