Optimization of a Potent, Orally Active S1P1 Agonist Containing a Quinolinone Core

Paul E Harrington; Michael D Croghan; Christopher Fotsch; Mike Frohn; Brian A Lanman; Lewis D Pennington; Alexander J Pickrell; Anthony B Reed; Kelvin K C Sham; Andrew Tasker; Heather A Arnett; Michael Fiorino; Matthew R Lee; Michele McElvain; Henry G Morrison; Han Xu; Yang Xu; Xuxia Zhang; Min Wong; Victor J Cee

doi:10.1021/ml200252b

Optimization of a Potent, Orally Active S1P1 Agonist Containing a Quinolinone Core

ACS Med Chem Lett. 2011 Nov 23;3(1):74-8. doi: 10.1021/ml200252b. eCollection 2012 Jan 12.

Authors

Paul E Harrington¹, Michael D Croghan¹, Christopher Fotsch¹, Mike Frohn¹, Brian A Lanman¹, Lewis D Pennington¹, Alexander J Pickrell¹, Anthony B Reed¹, Kelvin K C Sham¹, Andrew Tasker¹, Heather A Arnett¹, Michael Fiorino¹, Matthew R Lee¹, Michele McElvain¹, Henry G Morrison¹, Han Xu¹, Yang Xu¹, Xuxia Zhang¹, Min Wong¹, Victor J Cee¹

Affiliation

¹ Chemistry Research and Discovery, Inflammation Research, Molecular Structure, HTS and Molecular Pharmacology, Pharmaceutics, and Pharmacokinetics and Drug Metabolism, Amgen , One Amgen Center Drive, Thousand Oaks, California 91320-1799, United States.

Abstract

The optimization of a series of S1P1 agonists with limited activity against S1P3 is reported. A polar headgroup was used to improve the physicochemical and pharmacokinetic parameters of lead quinolinone 6. When dosed orally at 1 and 3 mg/kg, the azahydroxymethyl analogue 22 achieved statistically significant lowering of circulating blood lymphocytes 24 h postdose. In rats, a dose-proportional increase in exposure was measured when 22 was dosed orally at 2 and 100 mg/kg.

Keywords: S1P1; Sphingosine-1-phosphate receptor; agonist; multiple sclerosis.