• Title of article

    3-Oxa-15-cyclohexyl prostaglandin DP receptor agonists as topical antiglaucoma agents Original Research Article

  • Author/Authors

    Mark R. Hellberg، نويسنده , , Raymond E. Conrow، نويسنده , , Najam A. Sharif، نويسنده , , Marsha A. McLaughlin، نويسنده , , John E. Bishop، نويسنده , , Julie Y. Crider، نويسنده , , W Dennis Dean، نويسنده , , Kevin A. DeWolf، نويسنده , , David R. Pierce، نويسنده , , Verney L. Sallee، نويسنده , , Robert D. Selliah، نويسنده , , Bryon S. Severns، نويسنده , , Steven J. Sproull، نويسنده , , Gary W. Williams، نويسنده , , Paul W. Zinke، نويسنده , , Peter G. Klimko، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2002
  • Pages
    19
  • From page
    2031
  • To page
    2049
  • Abstract
    A series of prostaglandin DP agonists containing a 3-oxa-15-cyclohexyl motif was synthesized and evaluated in several in vitro and in vivo biological assays. The reference compound ZK 118.182 (9β-chloro-15-cyclohexyl-3-oxa-ω-pentanor PGF2α) is a potent full agonist at the prostaglandin DP receptor. Saturation of the 13,14 olefin affords AL-6556, which is less potent but is still a full agonist. Replacement of the 9-chlorine with a hydrogen atom or inversion of the carbon 15 stereochemistry also reduces affinity. In in vivo studies ZK 118.182 lowers intraocular pressure (IOP) upon topical application in the ocular hypertensive monkey. Ester, 1-alcohol, and selected amide prodrugs of the carboxylic acid enhance in vivo potency, presumably by increasing bioavailability. The clinical candidate AL–6598, the isopropyl ester prodrug of AL-6556, produces a maximum 53% drop in monkey IOP with a 1 μg dose (0.003% w/w) using a twice-daily dosing regime. Synthetically, AL–6598 was accessed from known intermediate 1 using a novel key sequence to install the cis allyl ether in the α chain, involving a selective Swern oxidative desilylation of a primary silyl ether in the presence of a secondary silyl ether. In this manner, 136 g of AL–6598 was synthesized under GMP conditions for evaluation in phase I clinical trials.
  • Journal title
    Bioorganic and Medicinal Chemistry
  • Serial Year
    2002
  • Journal title
    Bioorganic and Medicinal Chemistry
  • Record number

    1302134