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PDBsum entry 2asg
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Membrane protein
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PDB id
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2asg
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References listed in PDB file
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Key reference
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Title
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Interaction of noncompetitive inhibitors with an immobilized alpha3beta4 nicotinic acetylcholine receptor investigated by affinity chromatography, Quantitative-Structure activity relationship analysis, And molecular docking.
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Authors
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K.Jozwiak,
S.Ravichandran,
J.R.Collins,
I.W.Wainer.
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Ref.
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J Med Chem, 2004,
47,
4008-4021.
[DOI no: ]
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PubMed id
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Abstract
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A large number of drug substances act as noncompetitive inhibitors (NCIs) of the
nicotinic acetylcholine receptor (nAChR) by blocking the ion flux through the
channel. An affinity chromatography technique has been developed for
investigating the interactions between NCIs and the alpha3beta4 subtype of
neuronal nAChR. The data obtained from the chromatographic study were used to
construct QSAR models of the NCI-nAChR binding with both electronic and steric
parameters observed as important descriptors. A molecular model of the
transmembrane domain of the alpha3beta4 subtype of nAChR was constructed and
used to simulate the docking of a series of NCIs. A key aspect of the model was
the discovery of the cleft produced by the incorporation of the bulky
phenylalanine moiety into the nonpolar section of the lumen by the beta4
subunit. Quantitatively, the results of docking simulations modeled the
experimental affinity data better than QSAR results. The computational approach,
combined with the modeling of NCI-nAChR interaction by affinity chromatography,
can be used to predict possible toxicities and adverse interactions.
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