2015
DOI: 10.1039/c5ra10812h
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Binding mechanism of nine N-phenylpiperazine derivatives and α1A-adrenoceptor using site-directed molecular docking and high performance affinity chromatography

Abstract: Investigating the binding mechanism of α1A-adrenoceptor and its specific ligands by affinity chromatography.

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Cited by 6 publications
(3 citation statements)
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“…Moreover, the possibility of hydrophobic interactions can be operative and decisive also. Quite interestingly, these interactions were in line with the binding mechanism predicted by molecular docking for the interaction of [mCPP] + with serotonin receptor subtypes "5-HT 1A receptor", a major target for research and drug development due to its implication in many physiological processes [41] as well as with the adrenergic receptor; α 1A -adrenoceptor [42]. Furthermore, the piperazine core acts as a hydrogen bonding donating site with crown ether-oxygen atoms through N-H .…”
Section: Membrane Response and Sensitivity Of The Sensorssupporting
confidence: 71%
“…Moreover, the possibility of hydrophobic interactions can be operative and decisive also. Quite interestingly, these interactions were in line with the binding mechanism predicted by molecular docking for the interaction of [mCPP] + with serotonin receptor subtypes "5-HT 1A receptor", a major target for research and drug development due to its implication in many physiological processes [41] as well as with the adrenergic receptor; α 1A -adrenoceptor [42]. Furthermore, the piperazine core acts as a hydrogen bonding donating site with crown ether-oxygen atoms through N-H .…”
Section: Membrane Response and Sensitivity Of The Sensorssupporting
confidence: 71%
“…4 A and B) both positioned in the hydrophobic pocket involving TM 2, 3, 6 and 7 with the same calculated binding energies (—9.0 kcal/mol). The OH group of ( R )-NAF formed a hydrogen bond (2.6 Å) with Glu190 in the ECL2 region that has been reported to be essential for GPCR activation 23 . The methoxyl at the arylpiperazine moiety formed an H-bond with Thr189 (3.0 Å between the oxygen atom of methoxyl group and the hydroxyl oxygen atom of Thr189).…”
Section: Resultsmentioning
confidence: 99%
“…High-performance affinity chromatography (HPAC) , has been realized as an alternative method for rapid drug–protein interaction analysis with the advantages of good stability and reproducibility, low consumption of protein, and large number of samplings. To pursue the drug–protein interaction, HPAC is commonly performed by frontal analysis and zonal elution . The two methods are often challenged by the relatively long analysis time and the use of large amounts of drugs as they require saturation of the column by the analytes. , Such issues are partly addressed by nonlinear chromatography, injection amount-dependent assay, and peak profiling approaches. , However, most of the cases have concentrated on the bindings of drugs to serum albumin whereby their feasibility in the other systems remains elusive.…”
Section: Introductionmentioning
confidence: 99%