New nonpeptide angiotensin II receptor antagonists. 2. Synthesis, biological properties, and structure-activity relationships of 2-alkyl-4-(biphenylylmethoxy)quinoline derivatives

Bradbury, Robert H.; Allott, Christopher P.; Dennis, Michael Robert; Fisher, Eric; Major, John S.; Masek, Brian B.; Oldham, Alec A.; Pearce, R.; Rankine, Neil

doi:10.1021/jm00100a007

Cited by 55 publications

(26 citation statements)

References 4 publications

(7 reference statements)

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“…The two rings of the biphenyl moiety of the molecule were found to prefer a twisted conformation. Such a conformation is consistent with a subsequently reported crystallographic structure of EXP7711, an o-carboxyl acid analogue of losartan [38]. The molecule adopts a V-shape with the otetrazole group folded back towards the n-butyl group.…”

Section: Resultssupporting

confidence: 89%

Superimposition of potent non-peptide AT1 receptor antagonists with angiotensin II

et al. 1996

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The model of angiotensin II (ANG II) developed in our laboratory using a combination of NMR, fluorescence data and molecular graphics [Matsoukas, J.M. et al., J. Biol. Chem., 269 (1994) 5303] served as a template for a systematic superimposition of potent AT~ receptor antagonists with ANG II. The key amino acids in this model, tyrosine, phenylalanine and histidine, form a charge-relay system. The studied ANG II AT~ receptor antagonists were found to accommodate this relay system. The proposed model offers a motivation to synthetic chemists to develop ANG II antagonists that differ from the losartan prototype structure but possess an enhanced biological profile.

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Section: Resultssupporting

confidence: 89%

Superimposition of potent non-peptide AT1 receptor antagonists with angiotensin II

et al. 1996

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“…(Note that only four out of 12 750 initial conformers of L-158809 need to be considered with regard to the receptor-bound conformation when the final OMAP is imposed.) Other workers have attempted to describe the conformation of antagonists bound to A-II [23]. The conformation we chose to carry through the CoMFA analysis resembles the 'Helix 1' (H1) geometry with regard to the heterocycle-phenyl torsions [23d].…”

Section: Resultsmentioning

confidence: 99%

Derivation of a 3D pharmacophore model for the angiotensin-II site one receptor

Prendergast

Adams²,

Greenlee³

et al. 1994

J Computer-Aided Mol Des

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A systematic search has been used to derive a hypothesis for the receptor-bound conformation of A-II antagonists at the AT1 receptor. The validity of the pharmacophore hypothesis has been tested using CoMFA, which included 50 diverse A-II antagonists, spanning four orders of magnitude in activity. The resulting cross-validated R2 of 0.64 (conventional R2 of 0.76) is indicative of a good predictive model of activity, and has been used to estimate potency for a variety of non-peptidyl antagonists. The structural model for the non-peptide has been compared with respect to the natural substrate, A-II, by generating peptide to non-peptide overlays.

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“…The Ang II receptor antagonistic activity data of 2-alkyl 4-(biphenylylmethoxy)quinolines were taken from the reported work of Bradbury et al [8] (Table 1). The biological activity data (IC 50 in µM) was converted to negative logarithmic mole dose (pIC 50 ) for quantitative structure activity relationship (QSAR) analysis.…”

Section: Methodsmentioning

confidence: 99%

Insight into the Structural Requirement of 2-Alkyl-4-(biphenylmethoxy)quinolines as Nonpeptide Angiotensin II Receptor Antagonists: A QSAR Approach

Vyas

2009

Sci. Pharm.

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In the current study a quantitative structure activity relationship approach using sequential multiple linear regression analysis was applied to a series of 2-alkyl-4-(biphenylylmethoxy)quinolines as angiotensin II (Ang II) receptor antagonists by using Chem 3D and Dragon Software. The studies, carried out on 33 analogs, give statistically significant correlations of selective Ang II antagonistic activity with physical properties concerning size, symmetry, shape and distribution of molecule atoms. Among several 2D quantitative structure activity relationship models, one model gave good statistical significance (r > 0.81, Ftest = 10.47, S < 0.30, chance correlation < 0.01). 3D QSAR studies show that Hennery's law constant, Dipole and VDWE play a significant role in Ang II antagonistic activity. These QSAR studies help us in the design and prediction of novel substituted benzimidazole Ang II receptor antagonists. Keywords

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New nonpeptide angiotensin II receptor antagonists. 2. Synthesis, biological properties, and structure-activity relationships of 2-alkyl-4-(biphenylylmethoxy)quinoline derivatives

Cited by 55 publications

References 4 publications

Superimposition of potent non-peptide AT1 receptor antagonists with angiotensin II

Superimposition of potent non-peptide AT1 receptor antagonists with angiotensin II

Derivation of a 3D pharmacophore model for the angiotensin-II site one receptor

Insight into the Structural Requirement of 2-Alkyl-4-(biphenylmethoxy)quinolines as Nonpeptide Angiotensin II Receptor Antagonists: A QSAR Approach

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