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Stereochemical Requirements for the Mineralocorticoid Receptor Antagonist Activity of Dihydropyridines

  作者 ARHANCET GRACIELA B; WOODARD SCOTT S; DIETZ JESSICA D; GARLAND DANNY J; WAGNER GRACE M; IYANAR KALIAPPAN; COLLINS JOE T; BLINN JAMES R; NUMANN RANDAL E; HU XIAO; HUANG HORNGCHIH  
  选自 期刊  Journal of Medicinal Chemistry;  卷期  2010年53-10;  页码  4300-4304  
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[摘要]A number of known 1,4-dihydropyridine CCBs were identified as having comparable potency to the steroidal MR antagonist eplerenone. Chiral resolution of mebudipine revealed that MR and CCB activity reside in opposite enantiomers. Small molecule X-ray crystal structures showed that the C4 stereochemistry of optimized selective MR analogues, e.g. 5, is consistent with MR-active mebudipine. Molecular modeling supports a binding pose consistent with that previously proposed for DHP diesters.

 
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