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Discovery of Highly Potent Liver X Receptor ß Agonists.
Kick, Ellen K; Busch, Brett B; Martin, Richard; Stevens, William C; Bollu, Venkataiah; Xie, Yinong; Boren, Brant C; Nyman, Michael C; Nanao, Max H; Nguyen, Lam; Plonowski, Artur; Schulman, Ira G; Yan, Grace; Zhang, Huiping; Hou, Xiaoping; Valente, Meriah N; Narayanan, Rangaraj; Behnia, Kamelia; Rodrigues, A David; Brock, Barry; Smalley, James; Cantor, Glenn H; Lupisella, John; Sleph, Paul; Grimm, Denise; Ostrowski, Jacek; Wexler, Ruth R; Kirchgessner, Todd; Mohan, Raju.
Affiliation
  • Kick EK; Department of Discovery Chemistry, Department of Cardiovascular Biology, Pharmaceutical Candidate Optimization, Research & Development, Bristol-Myers Squibb , P.O. Box 5400, Princeton, New Jersey 08543-5400, United States.
  • Busch BB; Exelixis Inc. , 210 East Grand Avenue, South San Francisco, California 94080, United States.
  • Martin R; Exelixis Inc. , 210 East Grand Avenue, South San Francisco, California 94080, United States.
  • Stevens WC; Exelixis Inc. , 210 East Grand Avenue, South San Francisco, California 94080, United States.
  • Bollu V; Exelixis Inc. , 210 East Grand Avenue, South San Francisco, California 94080, United States.
  • Xie Y; Exelixis Inc. , 210 East Grand Avenue, South San Francisco, California 94080, United States.
  • Boren BC; Exelixis Inc. , 210 East Grand Avenue, South San Francisco, California 94080, United States.
  • Nyman MC; Exelixis Inc. , 210 East Grand Avenue, South San Francisco, California 94080, United States.
  • Nanao MH; Exelixis Inc. , 210 East Grand Avenue, South San Francisco, California 94080, United States.
  • Nguyen L; Exelixis Inc. , 210 East Grand Avenue, South San Francisco, California 94080, United States.
  • Plonowski A; Exelixis Inc. , 210 East Grand Avenue, South San Francisco, California 94080, United States.
  • Schulman IG; Exelixis Inc. , 210 East Grand Avenue, South San Francisco, California 94080, United States.
  • Yan G; Exelixis Inc. , 210 East Grand Avenue, South San Francisco, California 94080, United States.
  • Zhang H; Department of Discovery Chemistry, Department of Cardiovascular Biology, Pharmaceutical Candidate Optimization, Research & Development, Bristol-Myers Squibb , P.O. Box 5400, Princeton, New Jersey 08543-5400, United States.
  • Hou X; Department of Discovery Chemistry, Department of Cardiovascular Biology, Pharmaceutical Candidate Optimization, Research & Development, Bristol-Myers Squibb , P.O. Box 5400, Princeton, New Jersey 08543-5400, United States.
  • Valente MN; Department of Discovery Chemistry, Department of Cardiovascular Biology, Pharmaceutical Candidate Optimization, Research & Development, Bristol-Myers Squibb , P.O. Box 5400, Princeton, New Jersey 08543-5400, United States.
  • Narayanan R; Department of Discovery Chemistry, Department of Cardiovascular Biology, Pharmaceutical Candidate Optimization, Research & Development, Bristol-Myers Squibb , P.O. Box 5400, Princeton, New Jersey 08543-5400, United States.
  • Behnia K; Department of Discovery Chemistry, Department of Cardiovascular Biology, Pharmaceutical Candidate Optimization, Research & Development, Bristol-Myers Squibb , P.O. Box 5400, Princeton, New Jersey 08543-5400, United States.
  • Rodrigues AD; Department of Discovery Chemistry, Department of Cardiovascular Biology, Pharmaceutical Candidate Optimization, Research & Development, Bristol-Myers Squibb , P.O. Box 5400, Princeton, New Jersey 08543-5400, United States.
  • Brock B; Department of Discovery Chemistry, Department of Cardiovascular Biology, Pharmaceutical Candidate Optimization, Research & Development, Bristol-Myers Squibb , P.O. Box 5400, Princeton, New Jersey 08543-5400, United States.
  • Smalley J; Department of Discovery Chemistry, Department of Cardiovascular Biology, Pharmaceutical Candidate Optimization, Research & Development, Bristol-Myers Squibb , P.O. Box 5400, Princeton, New Jersey 08543-5400, United States.
  • Cantor GH; Department of Discovery Chemistry, Department of Cardiovascular Biology, Pharmaceutical Candidate Optimization, Research & Development, Bristol-Myers Squibb , P.O. Box 5400, Princeton, New Jersey 08543-5400, United States.
  • Lupisella J; Department of Discovery Chemistry, Department of Cardiovascular Biology, Pharmaceutical Candidate Optimization, Research & Development, Bristol-Myers Squibb , P.O. Box 5400, Princeton, New Jersey 08543-5400, United States.
  • Sleph P; Department of Discovery Chemistry, Department of Cardiovascular Biology, Pharmaceutical Candidate Optimization, Research & Development, Bristol-Myers Squibb , P.O. Box 5400, Princeton, New Jersey 08543-5400, United States.
  • Grimm D; Department of Discovery Chemistry, Department of Cardiovascular Biology, Pharmaceutical Candidate Optimization, Research & Development, Bristol-Myers Squibb , P.O. Box 5400, Princeton, New Jersey 08543-5400, United States.
  • Ostrowski J; Department of Discovery Chemistry, Department of Cardiovascular Biology, Pharmaceutical Candidate Optimization, Research & Development, Bristol-Myers Squibb , P.O. Box 5400, Princeton, New Jersey 08543-5400, United States.
  • Wexler RR; Department of Discovery Chemistry, Department of Cardiovascular Biology, Pharmaceutical Candidate Optimization, Research & Development, Bristol-Myers Squibb , P.O. Box 5400, Princeton, New Jersey 08543-5400, United States.
  • Kirchgessner T; Department of Discovery Chemistry, Department of Cardiovascular Biology, Pharmaceutical Candidate Optimization, Research & Development, Bristol-Myers Squibb , P.O. Box 5400, Princeton, New Jersey 08543-5400, United States.
  • Mohan R; Exelixis Inc. , 210 East Grand Avenue, South San Francisco, California 94080, United States.
ACS Med Chem Lett ; 7(12): 1207-1212, 2016 Dec 08.
Article in En | MEDLINE | ID: mdl-27994765
ABSTRACT
Introducing a uniquely substituted phenyl sulfone into a series of biphenyl imidazole liver X receptor (LXR) agonists afforded a dramatic potency improvement for induction of ATP binding cassette transporters, ABCA1 and ABCG1, in human whole blood. The agonist series demonstrated robust LXRß activity (>70%) with low partial LXRα agonist activity (<25%) in cell assays, providing a window between desired blood cell ABCG1 gene induction in cynomolgus monkeys and modest elevation of plasma triglycerides for agonist 15. The addition of polarity to the phenyl sulfone also reduced binding to the plasma protein, human α-1-acid glycoprotein. Agonist 15 was selected for clinical development based on the favorable combination of in vitro properties, excellent pharmacokinetic parameters, and a favorable lipid profile.
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Full text: 1 Collection: 01-internacional Database: MEDLINE Language: En Journal: ACS Med Chem Lett Year: 2016 Document type: Article Affiliation country: Estados Unidos
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Full text: 1 Collection: 01-internacional Database: MEDLINE Language: En Journal: ACS Med Chem Lett Year: 2016 Document type: Article Affiliation country: Estados Unidos