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Exploring monocyclic core: Discovery of pyrrol-2-one derivatives as a new series of potent MCHR1 antagonists with in vivo efficacy.
A M Subbaiah, Murugaiah; Mandal, Umasankar; Patankar, Vidya; Bhaskaran, Selvakumar; Nutakki, Ravikumar; Rami, Bhadresh; Shah, Devang Praful; Mahammad, Shahe; Murphy, Brian J; Huang, Christine; Robl, Jeffrey A; Washburn, William N.
Afiliação
  • A M Subbaiah M; Department of Medicinal Chemistry, Biocon-Bristol Myers Squibb Research and Development Centre, Biocon Park, Bommasandra IV Phase, Jigani Link Road, Bangalore, PIN 560099, Karnataka, India. Electronic address: murugaiah.subbaiah123@gmail.com.
  • Mandal U; Department of Medicinal Chemistry, Biocon-Bristol Myers Squibb Research and Development Centre, Biocon Park, Bommasandra IV Phase, Jigani Link Road, Bangalore, PIN 560099, Karnataka, India.
  • Patankar V; Department of Medicinal Chemistry, Biocon-Bristol Myers Squibb Research and Development Centre, Biocon Park, Bommasandra IV Phase, Jigani Link Road, Bangalore, PIN 560099, Karnataka, India.
  • Bhaskaran S; Department of Medicinal Chemistry, Biocon-Bristol Myers Squibb Research and Development Centre, Biocon Park, Bommasandra IV Phase, Jigani Link Road, Bangalore, PIN 560099, Karnataka, India.
  • Nutakki R; Department of Biology, Biocon-Bristol Myers Squibb Research and Development Centre, Biocon Park, Bommasandra IV Phase, Jigani Link Road, Bangalore, PIN 560099, Karnataka, India.
  • Rami B; Department of Biology, Biocon-Bristol Myers Squibb Research and Development Centre, Biocon Park, Bommasandra IV Phase, Jigani Link Road, Bangalore, PIN 560099, Karnataka, India.
  • Shah DP; Department of Pharmaceutical Candidate Optimization, Biocon-Bristol Myers Squibb Research and Development Centre, Biocon Park, Bommasandra IV Phase, Jigani Link Road, Bangalore, PIN 560099, Karnataka, India.
  • Mahammad S; Department of Biopharmaceutics, Biocon-Bristol Myers Squibb Research and Development Centre, Biocon Park, Bommasandra IV Phase, Jigani Link Road, Bangalore, PIN 560099, Karnataka, India.
  • Murphy BJ; Department of Metabolic Diseases Biology, Bristol Myers Squibb Research and Early Development, PO Box 4000, Princeton, NJ, 08543-4000, USA.
  • Huang C; Department of Pharmaceutical Candidate Optimization, Bristol Myers Squibb Research and Early Development, PO Box 4000, Princeton, NJ, 08543-4000, USA.
  • Robl JA; Department of Metabolic Diseases Chemistry, Bristol Myers Squibb Research and Early Development, PO Box 4000, Princeton, NJ, 08543-4000, USA.
  • Washburn WN; Department of Metabolic Diseases Chemistry, Bristol Myers Squibb Research and Early Development, PO Box 4000, Princeton, NJ, 08543-4000, USA.
Eur J Med Chem ; 276: 116686, 2024 Oct 05.
Article em En | MEDLINE | ID: mdl-39053192
ABSTRACT
With an objective to improve the profiles of the 1st generation non-basic MCHR1 antagonists, a lean design approach of replacing the bicyclic thienopyrimidine core with a monocyclic pyrrol-2-one chemotype was examined in the context of reducing aromatic ring count, while also contemplating enhanced flexibility as a means of decreasing flat character. The new compounds exhibited potent antagonism up to the sub-nanomolar range, thereby implying that the monocyclic ring could effectively serve as an effective bioisostere of the bicyclic system. The prototype compound 2m offered benefits like improved potency, reduced half-life, and enhanced solubility, while also demonstrating >5% reduction in weight gain in rats, thereby providing proof-of-concept for this new class of compounds as anti-obesity agents.
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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Pirróis Idioma: En Ano de publicação: 2024 Tipo de documento: Article
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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Pirróis Idioma: En Ano de publicação: 2024 Tipo de documento: Article