Synthesis and biological activities of turkesterone 11α-acyl derivatives | Zendy

Laurence Dinan | Zendy; Pauline Bourne | Zendy; Pensri Whiting | Zendy; Ada Tsitsekli | Zendy; Z. Saatov | Zendy; Tarlochan S. Dhadialla | Zendy; Robert E. Hormann | Zendy; René Lafont | Zendy; Josep Coll | Zendy

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Synthesis and biological activities of turkesterone 11α-acyl derivatives

Author(s) -

Laurence Dinan,

Pauline Bourne,

Pensri Whiting,

Ada Tsitsekli,

Z. Saatov,

Tarlochan S. Dhadialla,

Robert E. Hormann,

René Lafont,

Josep Coll

Publication year - 2003

Publication title -

journal of insect science

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.551

H-Index - 49

ISSN - 1536-2442

DOI - 10.1093/jis/3.1.6

Subject(s) - biology

Turkesterone is a phytoecdysteroid possessing an 11α-hydroxyl group. It is an analogue of the insect steroid hormone 20-hydroxyecdysone. Previous ecdysteroid QSAR and molecular modelling studies predicted that the cavity of the ligand binding domain of the ecdysteroid receptor would possess space in the vicinity of C-11/C-12 of the ecdysteroid. We report the regioselective synthesis of a series of turkesterone 11α-acyl derivatives in order to explore this possibility. The structures of the analogues have been unambiguously determined by spectroscopic means (NMR and low-resolution mass spectrometry). Purity was verified by HPLC. Biological activities have been determined in Drosophila melanogaster BII cell-based bioassay for ecdysteroid agonists and in an in vitro radioligand-displacement assay using bacterially-expressed D. melanogaster EcR/USP receptor proteins. The 11α-acyl derivatives do retain a significant amount of biological activity relative to the parent ecdysteroid. Further, although activity initially drops with the extension of the acyl chain length (C2 to C4), it then increases (C6 to C10), before decreasing again (C14 and C20). The implications of these findings for the interaction of ecdysteroids with the ecdysteroid receptor and potential applications in the generation of affinity-labelled and fluorescently-tagged ecdysteroids are discussed.Abbreviation:CoMFA comparative molecular field analysisDCM dichloromethaneDMF dimethylformamideDMP 2,2-dimethoxypropane4D-QSAR 4-dimensional quantitative structure-activity relationshipEcR ecdysteroid receptorEcRE ecdysteroid response elementHPLC high-performance liquid chromatographyLBD ligand-binding domainNMR nuclear magnetic resonanceponA ponasterone AQSAR quantitative structure-activity relationshipRXR retinoid X receptorSAR structure-activity relationshipSPE solid-phase extractionTHF tetrahydrofuranTLC thin-layer chromatographyp-TsOH para-toluenesulphonic acidUSP ultraspiracleUV-VIS ultraviolet-visible

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