Your search keyword '"Phendioxan"' showing total 2 results

1. Structure−Activity Relationships in 1,4-Benzodioxan-Related Compounds. 8. {2-[2-(4-Chlorobenzyloxy)phenoxy]ethyl}-[2-(2,6-dimethoxyphenoxy)ethyl]amine (Clopenphendioxan) as a Tool to Highlight the Involvement of α1D- and α1B-Adrenoreceptor Subtypes in the Regulation of Human PC-3 Prostate Cancer Cell Apoptosis and Proliferation

Author

Michela Mosca, Michela Buccioni, Francesco Gentili, Giorgio Santoni, Massimo Nabissi, and Amedeo Leonardi, Alessandro Piergentili, Patrizia Ballarini, Roberta Lucciarini, Consuelo Amantini, Mario Giannella, Elena Poggesi, Maria Pigini, and Wilma Quaglia

Subjects

Chemistry, Stereochemistry, Cell growth, Sulforhodamine B, Pharmacology, chemistry.chemical_compound, Benzodioxan, Cell culture, Apoptosis, Drug Discovery, Molecular Medicine, Structure–activity relationship, Phendioxan, Cytotoxicity

Abstract

A series of new α1-adrenoreceptor antagonists (5−18) was prepared by introducing various substituents (Topliss approach) into the ortho, meta, and para positions of the benzyloxy function of the phendioxan open analogue 4 (“openphendioxan”). All the compounds synthesized were potent antagonists and generally displayed, similarly to 4, the highest affinity values at α1D- with respect to α1A- and α1B-AR subtypes and 5-HT1A subtype. By sulforhodamine B (SRB) assay on human PC-3 prostate cancer cells, the new compounds showed antitumor activity (estimated on the basis of three parameters GI50, TGI, LC50), at low micromolar concentration, with 7 (“clopenphendioxan”) exhibiting the highest efficacy. Moreover, this study highlighted for the first time α1D- and α1B-AR expression in PC3 cells and also demonstrated the involvement of these subtypes in the modulation of apoptosis and cell proliferation. A significant reduction of α1D- and α1B-AR expression in PC3 cells was associated with the apoptosis induced by 7....

Published

2005

2. Structure-activity relationships in 1,4-benzodioxan-related compounds. 4. Effect of aryl and alkyl substituents at position 3 on .alpha.-adrenoreceptor blocking activity

Author

Mario Giannella, Wilma Quaglia, Seyed Khosrow Tayebati, Alessandro Piergentili, Maria Pigini, Carlo Melchiorre, and Gabriella Marucci

Subjects

Male, Stereochemistry, Alpha (ethology), Stereoisomerism, In Vitro Techniques, Clonidine, Dioxanes, Norepinephrine, Structure-Activity Relationship, chemistry.chemical_compound, Vas Deferens, Drug Discovery, Animals, Moiety, Phendioxan, Adrenergic alpha-Antagonists, Bicyclic molecule, Chemistry, Aryl, Muscle, Smooth, Rats, Benzodioxan, Molecular Medicine, Isopropyl, Muscle Contraction

Abstract

The observation that the insertion of a phenyl ring at position 3 of WB 4101 (1) afforded a potent and selective alpha 1-adrenoreceptor antagonist, phendioxan (2), prompted us to further investigate that position of the 2,3-dihydro-1,4-benzodioxin moiety. Thus the 3-phenyl of 2 was replaced by methyl, isopropyl, cyclohexyl, or para-substituted phenyl groups either in a cis or a trans relationships affording compounds 3-17 and 58. The structure of these new derivatives was assigned on the basis of the coupling constant of hydrogens at positions 2 and 3 and confirmed by a crystallographic study. The blocking activity and relative selectivity of 3-17 on alpha 1- and alpha 2-adrenoreceptors were evaluated in the isolated rat vas deferens. The results were compared with those obtained for 1 and 2. All the compounds, with the exception of isopropyl and cyclohexyl derivatives 5-8, were effective alpha 1-adrenoreceptor antagonists with a significant alpha 1/alpha 2-selectivity. The lipophilic and/or electronic character of para substituents of the 3-phenyl ring does not alter markedly the affinity toward alpha 1-adrenoreceptors. However, the 3-p-tolyl derivative 10 was slightly more potent and even more selective than 2.

Published

1993