6-Acylamino-2-aminoquinolines as Potent Melanin-Concentrating Hormone 1 Receptor Antagonists. Identification, Structure−Activity Relationship, and Investigation of Binding Mode

Ulven, Trond; Frimurer, Thomas M.; Receveur, Jean-Marie; Little, Paul B.; Rist, Øystein; Nørregaard, Pia K.; Högberg, Thomas

doi:10.1021/jm050103y

Cited by 54 publications

(27 citation statements)

References 47 publications

(56 reference statements)

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“…MCH1 receptor screening was performed by Ulven et al, using a set of HypoGen pharmacophore hypotheses [38]. Twenty five 3D pharmacophore hypotheses were generated based on 42 representative known ligands of the same scaffold.…”

Section: Ligand-based Screeningmentioning

confidence: 99%

G Protein Coupled Receptors - In Silico Drug Discovery and Design

Sela¹,

Golan²,

Strajbl³

et al. 2010

CTMC

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In silico drug discovery is a complex process requiring flexibility and ingenuity in method selection and a careful validation of work protocols. GPCR in silico drug discovery poses additional challenges due to the paucity of crystallographic data. This paper starts by reviewing selected GPCR in silico screening programs reported in the literature, including both structure-based and ligand-based approaches. Particular emphasis is given to library design, binding mode selection, process validation and compound selection for biological testing. Following literature review, we provide insights into in silico methodologies and process workflows used at EPIX to drive over 20 highly successful screening and lead optimization programs performed since 2001. Applications of the various methodologies discussed are demonstrated by examples from recent programs that have not yet been published.

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Section: Ligand-based Screeningmentioning

confidence: 99%

G Protein Coupled Receptors - In Silico Drug Discovery and Design

Sela¹,

Golan²,

Strajbl³

et al. 2010

CTMC

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“…7TM Pharma recently published a series of papers describing the discovery and optimization of their aminomethylquinoline and ureidobenzamide series (Receveur et al, 2004;Ulven et al, 2005;Ulven et al, 2006). Although this group was able to produce low nanomolar affinity compounds such as compounds 8 and 9 (See Fig.…”

Section: Development Of Small Molecule Mchr1 Antagonistsmentioning

confidence: 99%

Anti-obesity effects of small molecule melanin-concentrating hormone receptor1 (MCHR1) antagonists

Luthin

2007

Life Sciences

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“…46 Thus, modification of the benzamide group in bicyclic derivatives retaining a carbonyl group, was proposed as an effective strategy for minimizing clearance of the compounds. 47 However, in the case of the fused benzopyridazinones ring as compound 6 (Figure 8), the improved pharmacokinetics was also associated with some untoward partitioning of the compound into tissues and very high brain penetration. 48 Later, they showed a series of substituted chromones (compound 7, Figure 8) with subnanomolar binding affinity and 66% oral bioavailability in rats.…”

Section: Carboxamide Derivativesmentioning

confidence: 99%

“…antagonists; their design was structure-based on biphenyl carboxy group replacements suggesting key pharmacophoric points (a tertiary amine, an amide bond and a terminal aromatic ring of the biphenyl group) for biological activity. 47 Compound 9 ( Figure 10) showed its potential as an effective orally dosed MCH-R1 antagonist. Unfortunately, compound 9 was compromised by its hERG blockage activity, leading to an observed dose-dependent increase in QT interval in anesthetized dogs at serum concentrations comparable to those obtained at efficacious doses.…”

Section: Carboxamide Derivativesmentioning

confidence: 99%

MCH-R1 Antagonists as Potential Anti-obesity Drugs. Design Strategies and Structure-activity Relationship

Rivera¹,

Moreno²,

Bocanegra-García³

2013

Revista Virtual De Química

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Resumo:A obesidade é uma doença crônica que é caracterizada por um acúmulo de excesso de tecido adiposo. Atualmente, existem alguns medicamentos seguros e eficazes para o tratamento farmacológico da obesidade. Portanto, torna-se necessário o desenvolvimento de novas drogas. Na última década, o alvo mais promissor para a obesidade foi o hormônio concentrador de melanina. Com isso, diversas indústrias farmacêuticas desenvolveram peptídeos e pequenas moléculas como antagonistas MCH-R1, mas estes compostos apresentaram problemas como afinidade para o canal hERG e perfil farmacocinético pobre. Neste artigo, fizemos uma breve revisão da concepção da estratégia mais relevante e relações da estrutura-atividade no desenvolvimento de carboxamida, ureias, quinolina e derivados quinazolina como antagonistas MCH-R1. Palavras-chave:Antagonistas; hormônio concentrador de melanina; obesidade. AbstractObesity is a chronic disease that is characterized by an accumulation of excess adipose tissue. Actually, there are few safe and effective drugs for pharmacological treatment of obesity. Therefore, it becomes necessary the development of new drugs. In the last decade, the most promising target for obesity was melanin-concentrating hormone. Thereat, diverse pharmaceutical companies developed peptides and small molecules as MCH-R1 antagonists, but, these compounds had problems as affinity for hERG channel and poor pharmacokinetic profile. In this manuscript, we made a brief review of the most relevant strategy design and structure-activity relationships in the development of carboxamide, ureas, quinoline, and quinazoline derivatives as MCH-R1 antagonists.

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6-Acylamino-2-aminoquinolines as Potent Melanin-Concentrating Hormone 1 Receptor Antagonists. Identification, Structure−Activity Relationship, and Investigation of Binding Mode

Cited by 54 publications

References 47 publications

G Protein Coupled Receptors - In Silico Drug Discovery and Design

G Protein Coupled Receptors - In Silico Drug Discovery and Design

Anti-obesity effects of small molecule melanin-concentrating hormone receptor1 (MCHR1) antagonists

MCH-R1 Antagonists as Potential Anti-obesity Drugs. Design Strategies and Structure-activity Relationship

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