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      Structure-based design of inhibitors of coagulation factor XIa with novel P1 moieties.

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          Abstract

          Compound 2 was previously identified as a potent inhibitor of factor XIa lacking oral bioavailability. A structure-based approach was used to design analogs of 2 with novel P1 moieties with good selectivity profiles and oral bioavailability. Further optimization of the P1 group led to the identification of a 4-chlorophenyltetrazole P1 analog, which when combined with further modifications to the linker and P2' group provided compound 32 with FXIa Ki=6.7 nM and modest oral exposure in dogs.

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          Author and article information

          Journal
          Journal ID (iso-abbrev): Bioorg. Med. Chem. Lett.
          Title: Bioorganic & medicinal chemistry letters
          ISSN (Electronic): 1464-3405
          ISSN (Print): 0960-894X
          Publication date (Electronic): Apr 1 2015
          Volume: 25
          Issue: 7
          Affiliations
          [1 ] Bristol-Myers Squibb Company, Research and Development, 311 Pennington-Rocky Hill Rd., Pennington, NJ 08534, United States. Electronic address: donald.pinto@bms.com.
          [2 ] Bristol-Myers Squibb Company, Research and Development, 311 Pennington-Rocky Hill Rd., Pennington, NJ 08534, United States. Electronic address: joanne.smallheer@bms.com.
          [3 ] Bristol-Myers Squibb Company, Research and Development, 311 Pennington-Rocky Hill Rd., Pennington, NJ 08534, United States.
          Article
          Publisher Item ID: S0960-894X(15)00040-2
          DOI: 10.1016/j.bmcl.2015.01.028
          PubMed ID: 25728130
          SO-VID: 86fbd6c6-b44f-4a4a-824d-98b28b209b88
          Copyright © Copyright © 2015 Elsevier Ltd. All rights reserved.
          History

          Keywords: Anticoagulant,Bioavailability,Factor XIa,Serine protease,Thrombosis
          Data availability:
          Keywords: Anticoagulant, Bioavailability, Factor XIa, Serine protease, Thrombosis

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