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Structure-guided design of peptide-based tryptase inhibitors |
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| Authors: | McGrath Mary E Sprengeler Paul A Hirschbein Bernard Somoza John R Lehoux Isabelle Janc James W Gjerstad Erik Graupe Michael Estiarte Angeles Venkataramani Chandru Liu Yang Yee Robb Ho Joseph D Green Michael J Lee Chang-Sun Liu Liang Tai Vincent Spencer Jeffrey Sperandio David Katz Bradley A |
| Affiliation: | Celera Genomics, Inc., 180 Kimball Way, South San Francisco, California 94080, USA. mary.mcgrath@gilead.com |
| Abstract: | Improved peptide-based inhibitors of human beta tryptase were discovered using information gleaned from tripeptide library screening and structure-guided design methods, including fragment screening. Our efforts sought to improve this class of inhibitors by replacing the traditional Lys or Arg P1 element. The optimized compounds display low nanomolar potency against the mast cell target and several hundred-fold selectivity with respect to serine protease off targets. Thus, replacement of Lys/Arg at P1 in a peptide-like scaffold does not need to be accompanied by a loss in target affinity. |
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