Abstract
In this study four and five-feature pharmacophores for selective antagonists at each of the three α1-adrenoceptor (AR) subtypes were used to identify novel α1-AR subtype selective compounds in the National Cancer Institute and Tripos LeadQuest databases. 12 compounds were selected, based on diversity of structure, predicted high affinity and selectivity at the α1D- subtype compared to α1A- and α1B-ARs. 9 out of 12 of the tested compounds displayed affinity at the α1A and α1D -AR subtypes and 6 displayed affinity at all three α1-AR subtypes, no α1B-AR selective compounds were identified. 8 of the 9 compounds with α1-AR affinity were antagonists and one compound displayed partial agonist characteristics. This virtual screening has successfully identified an α1A/D-AR selective antagonist, with low μM affinity with a novel structural scaffold of a an isoquinoline fused three-ring system and good lead-like qualities ideal for further drug development. © 2011 Stoddart et al.
Cite
CITATION STYLE
Stoddart, E. S., Senadheera, S., MacDougall, I. J. A., Griffith, R., & Finch, A. M. (2011). A novel structural framework for α1a/d-adrenoceptor selective antagonists identified using subtype selective pharmacophores. PLoS ONE, 6(5). https://doi.org/10.1371/journal.pone.0019695
Register to see more suggestions
Mendeley helps you to discover research relevant for your work.