Late-stage optimization of a tercyclic class of S1P3-sparing, S1P1 receptor agonists

Joshua C Horan; Daniel Kuzmich; Pingrong Liu; Darren DiSalvo; John Lord; Can Mao; Tamara D Hopkins; Hui Yu; Christian Harcken; Raj Betageri; Melissa Hill-Drzewi; Lori Patenaude; Monica Patel; Kimberly Fletcher; Donna Terenzzio; Brian Linehan; Heather Xia; Mita Patel; Debbie Studwell; Craig Miller; Eugene Hickey; Jeremy I Levin; Dustin Smith; Raymond A Kemper; Louise K Modis; Lynne C Bannen; Diva S Chan; Morrison B Mac; Stephanie Ng; Yong Wang; Wei Xu; René M Lemieux

doi:10.1016/j.bmcl.2015.11.090

Late-stage optimization of a tercyclic class of S1P3-sparing, S1P1 receptor agonists

Bioorg Med Chem Lett. 2016 Jan 15;26(2):466-471. doi: 10.1016/j.bmcl.2015.11.090. Epub 2015 Nov 26.

Authors

Joshua C Horan¹, Daniel Kuzmich², Pingrong Liu², Darren DiSalvo², John Lord², Can Mao², Tamara D Hopkins², Hui Yu², Christian Harcken², Raj Betageri², Melissa Hill-Drzewi², Lori Patenaude³, Monica Patel², Kimberly Fletcher², Donna Terenzzio², Brian Linehan², Heather Xia², Mita Patel², Debbie Studwell⁴, Craig Miller², Eugene Hickey², Jeremy I Levin², Dustin Smith², Raymond A Kemper⁴, Louise K Modis³, Lynne C Bannen⁵, Diva S Chan⁵, Morrison B Mac⁵, Stephanie Ng⁵, Yong Wang⁵, Wei Xu⁵, René M Lemieux²

Affiliations

¹ Medicinal Chemistry, Boehringer Ingelheim Pharmaceuticals, 900 Ridgebury Rd, Ridgefield, CT 06877, United States. Electronic address: joshua.horan@proteostasis.com.
² Medicinal Chemistry, Boehringer Ingelheim Pharmaceuticals, 900 Ridgebury Rd, Ridgefield, CT 06877, United States.
³ Inflammation and Immunology, Boehringer Ingelheim Pharmaceuticals, 900 Ridgebury Rd, Ridgefield, CT 06877, United States.
⁴ Non-Clinical Drug Safety, Boehringer Ingelheim Pharmaceuticals, 900 Ridgebury Rd, Ridgefield, CT 06877, United States.
⁵ Medicinal Chemistry, Exelixis, 210 East Grand Avenue, South San Francisco, CA 94080, United States.

PMID: 26687487
DOI: 10.1016/j.bmcl.2015.11.090

Abstract

Poor solubility and cationic amphiphilic drug-likeness were liabilities identified for a lead series of S1P3-sparing, S1P1 agonists originally developed from a high-throughput screening campaign. This work describes the subsequent optimization of these leads by balancing potency, selectivity, solubility and overall molecular charge. Focused SAR studies revealed favorable structural modifications that, when combined, produced compounds with overall balanced profiles. The low brain exposure observed in rat suggests that these compounds would be best suited for the potential treatment of peripheral autoimmune disorders.

Keywords: Autoimmune; S1P1; S1P3; Solubility.

MeSH terms

Animals
Brain / metabolism
Glutamic Acid / metabolism
Hep G2 Cells
Humans
Hydrogen Bonding
Kinetics
Oxadiazoles / blood
Oxadiazoles / chemical synthesis
Oxadiazoles / pharmacology*
Rats
Receptors, Lysosphingolipid / agonists*
Solubility
Structure-Activity Relationship
Thiadiazoles / blood
Thiadiazoles / chemical synthesis
Thiadiazoles / pharmacology*

Substances

Oxadiazoles
Receptors, Lysosphingolipid
Thiadiazoles
Glutamic Acid