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Merck
  • Nonpeptide urotensin-II receptor antagonists: a new ligand class based on piperazino-phthalimide and piperazino-isoindolinone subunits.

Nonpeptide urotensin-II receptor antagonists: a new ligand class based on piperazino-phthalimide and piperazino-isoindolinone subunits.

Journal of medicinal chemistry (2009-09-08)
Edward C Lawson, Diane K Luci, Shyamali Ghosh, William A Kinney, Charles H Reynolds, Jenson Qi, Charles E Smith, Yuanping Wang, Lisa K Minor, Barbara J Haertlein, Tom J Parry, Bruce P Damiano, Bruce E Maryanoff
摘要

We have discovered two related chemical series of nonpeptide urotensin-II (U-II) receptor antagonists based on piperazino-phthalimide (5 and 6) and piperazino-isoindolinone (7) scaffolds. These structure types are distinctive from those of U-II receptor antagonist series reported in the literature. Antagonist 7a exhibited single-digit nanomolar potency in rat and human cell-based functional assays, as well as strong binding to the human U-II receptor. In advanced pharmacological testing, 7a blocked the effects of U-II in vitro in a rat aortic ring assay and in vivo in a rat ear-flush model. A discussion of U-II receptor antagonist pharmacophores is presented, and a specifically defined model is suggested from tricycle 13, which has a high degree of conformational constraint.

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Sigma-Aldrich
酞酰亚胺, ≥99%
Sigma-Aldrich
酞酰亚胺 钾盐, 98%
Sigma-Aldrich
酞酰亚胺 钾盐, purum, ≥99.0% (NT)