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Optimization of the Central Core of Indolinone-Acetic Acid-Based CRTH2 (DP2) Receptor Antagonists

  作者 CROSIGNANI STEFANO; JORANDLEBRUN CATHERINE; PAGE PATRICK; CAMPBELL GORDON; COLOVRAY VERONIQUE; MISSOTTEN MARC; HUMBERT YVES; CLEVA CHRISTOPHE; ARRIGHI JEANFRANCOIS; GAUDET MARILENE; JOHNSON ZOE; FERRO PAMELA; CHOLLET ANDRE  
  选自 期刊  ACS Medicinal Chemistry Letters;  卷期  2011年2-8;  页码  644-649  
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[摘要]New spiroindolinone antagonists of CRTH2 are described. Following identification of insufficient stability in human plasma as an important liability of the lead compounds, replacement of the spirosuccinimide core with a spirohydantoin or spiropyrrolidinone structure has yielded a compound that is fully stable in human plasma and with good potency in a human whole blood assay (IC(50) = 69 nM) but shows a much lower oral bioavailability (6-9% in rodents) than the earlier compounds. Successive optimization aimed at restoring an acceptable oral bioavailability has yielded compound (S)-17a, which exhibits both stability in human plasma and a good oral bioavailability in rat (37%) and mouse (39%). This compound is also active in a mouse model of ovalbumin-induced lung inflammation following oral dosing at 30 mg/kg.

 
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