Pharmacophoric Search and 3D-QSAR Comparative Molecular Field Analysis Studies on Agonists of Melatonin Sheep Receptors

Marot, Christophe; Chavatte, Philippe; Morin‐Allory, Luc; Viaud, Marie-Claude; Guillaumet, Gérald; Renard, Pierre; Lesieur, D.; Michel, Aurélia

doi:10.1021/jm980026p

Cited by 45 publications

(30 citation statements)

References 25 publications

(38 reference statements)

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“…However, the MT 2 /MT 1 selectivities were relatively similar in both series. While the non-OMe compound 62 was a potent antagonist (IC 50 (Figure 4), showed a profile of binding affinities similar to the other two tetracyclic series. Surprisingly, no agonistic activity was detected in the Xenopus assay in any of these compounds and all analogues including the methoxy and ethoxy derivatives were antagonists.…”

Section: Nm)mentioning

confidence: 85%

“…The tetralines were described generally as equipotent to the corresponding naphthalenes [48]. Other bioisosteric replacements of the indole ring of melatonin with a benzofuran and benzothiophene moiety (compounds 4 and 5 (Figure1), respectively) resulted in a slight loss in affinity [49,50]. However, substitution of the melatonin indole ring with benzimidazole, i.e.…”

Section: Structure-affinity Relationships Of Ligands For ML 1 (Mt 1 +mentioning

confidence: 99%

“…However, substitution of the melatonin indole ring with benzimidazole, i.e. the formal replacement of C3 with N, dramatically reduced binding affinity [50]. The minimal structural requirement for receptor recognition represent phenylalkyl amides, [51], exemplified by compound 6, which demonstrated remarkably high affinity (K i ϭ 5.5 nM) in chicken brain despite its simplicity.…”

Section: Structure-affinity Relationships Of Ligands For ML 1 (Mt 1 +mentioning

confidence: 99%

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Recent Advances in Melatonin Receptor Ligands

Zlotos

2005

Archiv der Pharmazie

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Melatonin is a hormone exerting its multiple actions mainly through two G-protein-coupled receptors MT(1) and MT(2). Exploring the physiological role of each of these subtypes requires subtype selective MT(1) and MT(2) ligands. While several MT(2)-selective ligands were developed in the 1990s, no selective agonists and antagonists for the MT(1) subtype were described. The present article reviews mela toninergic ligands developed in the current millennium focusing on subtype selective agents and on drug candidates. Notable compounds are the MT(1)-selective agonists 35 and 134, MT(1)-selective antagonists 117 and 131, MT(2)-selective agonists 58, 70, 79, 97 and 125, MT(2)-selective antagonists 27, 73 and 119, and the highly potent non-selective agonist 120. The non-selective agonists agomelatine 2, and ramelteon 87 are drug candidates as antidepressive agent and for the treatment of insomnia and circadian rhythm disfunction, respectively.

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Section: Nm)mentioning

confidence: 85%

Section: Structure-affinity Relationships Of Ligands For ML 1 (Mt 1 +mentioning

confidence: 99%

Section: Structure-affinity Relationships Of Ligands For ML 1 (Mt 1 +mentioning

confidence: 99%

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Recent Advances in Melatonin Receptor Ligands

Zlotos

2005

Archiv der Pharmazie

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“…The presence of the potent Hbond acceptor pyridyl nitrogen in 7-azaserotonin makes it biologically interesting, like 7-azaindole and its analogs [15]. It is also evident from the QSAR and photophysical study on 7-azamelatonin (which has similar structure as that of 7-azaserotonin) that it is a potential probe for receptor recognition [16,17]. As far as the authors are aware there is no such QSAR study on 7-azaserotonin, but the additional H-bond acceptor site in 7-azaserotonin compared to serotonin may enhance the ability of binding 7-azaserotonin to receptor site, so that the 7-azaserotonin may act as a potential agonist or antagonist of serotonin receptor.…”

Section: Introductionmentioning

confidence: 99%

Effect of pyridyl nitrogen on the conformational landscape of 7-azaserotonin: A computational study

Biswal¹,

Wategaonkar²

2009

Journal of Molecular Structure: THEOCHEM

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“…The electronic structure and reactivity of azaindoles have been the subject of many reviews [1-4] and original investigations [5][6][7][8][9][10]. Formally, azaindoles are the products of replacing one of the benzene ring carbon atoms with a nitrogen atom [1,11].…”

mentioning

confidence: 99%

Correlations of the physicochemical parameters of azaindoles with their reactions

Kereselidze

Pachuliya

Zarkuya

et al. 2006

Chem Heterocycl Compd

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Using the AM1 semiempirical quantum method the enthalpies of formation, ionization energies, electron affinities, energy differences between highest occupied and lowest unoccupied orbitals, atomic charges, bond orders, and dipole moments have been calculated for 4-, 5-, 6-, and 7-azaindoles. A correlation has been built up between the calculated physicochemical parameters and the Hammett para-substituent and inductive constants. The 1H to 7H proton transfer in 7-azaindole has been quantitatively described.

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Pharmacophoric Search and 3D-QSAR Comparative Molecular Field Analysis Studies on Agonists of Melatonin Sheep Receptors

Cited by 45 publications

References 25 publications

Recent Advances in Melatonin Receptor Ligands

Recent Advances in Melatonin Receptor Ligands

Effect of pyridyl nitrogen on the conformational landscape of 7-azaserotonin: A computational study

Correlations of the physicochemical parameters of azaindoles with their reactions

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