4-aroylpiperidines and 4-(α-hydroxyphenyl)piperidines as selective sigma-1 receptor ligands: synthesis, preliminary pharmacological evaluation and computational studies

Background Sigma (σ) receptors are membrane-bound proteins characterised by an unusual promiscuous ability to bind a wide variety of drugs and their high affinity for typical neuroleptic drugs, such as haloperidol, and their potential as alternative targets for antipsychotic agents. Sigma receptors...

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Published in:BMC chemistry 2016-08, Vol.10 (1), p.53-53, Article 53
Main Authors: Ikome, Hermia N., Ntie-Kang, Fidele, Ngemenya, Moses N., Tu, Zhude, Mach, Robert H., Efange, Simon M. N.
Format: Article
Language:English
Subjects:
Affinity
Chemical compounds
Chemistry
Chemistry and Materials Science
Chemistry/Food Science
Diseases
Drugs
Hydroxyl groups
Ligands
Organic and Medicinal Chemistry
Pharmaceutical sciences
Proteins
Receptors
Research Article
Selectivity
Sulfur
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Summary:Background Sigma (σ) receptors are membrane-bound proteins characterised by an unusual promiscuous ability to bind a wide variety of drugs and their high affinity for typical neuroleptic drugs, such as haloperidol, and their potential as alternative targets for antipsychotic agents. Sigma receptors display diverse biological activities and represent potential fruitful targets for therapeutic development in combating many human diseases. Therefore, they present an interesting avenue for further exploration. It was our goal to evaluate the potential of ring opened spipethiane ( 1 ) analogues as functional ligands (agonists) for σ receptors by chemical modification. Results Chemical modification of the core structure of the lead compound, ( 1 ), by replacement of the sulphur atom with a carbonyl group, hydroxyl group and 3-bromobenzylamine with the simultaneous presence of 4-fluorobenzoyl replacing the spirofusion afforded novel potent sigma-1 receptor ligands 7a–f , 8a–f and 9d–e . The sigma-1 receptor affinities of 7e , 8a and 8f were slightly lower than that of 1 and their selectivities for this receptor two to threefold greater than that of 1 . Conclusions It was found that these compounds have higher selectivities for sigma-1 receptors compared to 1 . Quantitatitive structure–activity relationship studies revealed that sigma-1 binding is driven by hydrophobic interactions. Graphical abstract Identified pharmacophore features for sigma binding.
ISSN:1752-153X
1752-153X
2661-801X
DOI:10.1186/s13065-016-0200-1