Non-basic azolotriazinone MCHR1 antagonists for the treatment of obesity: An empirical brain-exposures-driven candidate selection for in vivo efficacy studies

Pratik Devasthale; Wei Wang; James Mignone; Kishore Renduchintala; Sridhar Radhakrishnan; Jayanthi Dhanapal; Jagannath Selvaraj; Rajesh Kuppusamy; Mary Ann Pelleymounter; Daniel Longhi; Ning Huang; Neil Flynn; Anthony V Azzara; Kenneth Rohrbach; James Devenny; Suzanne Rooney; Michael Thomas; Susan Glick; Helen Godonis; Susan Harvey; Mary Jane Cullen; Hongwei Zhang; Christian Caporuscio; Paul Stetsko; Mary Grubb; Christine Huang; Lisa Zhang; Chris Freeden; Brian J Murphy; Jeffrey A Robl; William N Washburn

doi:10.1016/j.bmcl.2015.09.018

Non-basic azolotriazinone MCHR1 antagonists for the treatment of obesity: An empirical brain-exposures-driven candidate selection for in vivo efficacy studies

Bioorg Med Chem Lett. 2015 Oct 15;25(20):4412-8. doi: 10.1016/j.bmcl.2015.09.018. Epub 2015 Sep 8.

Authors

Pratik Devasthale¹, Wei Wang², James Mignone², Kishore Renduchintala³, Sridhar Radhakrishnan³, Jayanthi Dhanapal³, Jagannath Selvaraj³, Rajesh Kuppusamy³, Mary Ann Pelleymounter⁴, Daniel Longhi⁴, Ning Huang⁴, Neil Flynn⁴, Anthony V Azzara⁴, Kenneth Rohrbach⁴, James Devenny⁴, Suzanne Rooney⁴, Michael Thomas⁴, Susan Glick⁴, Helen Godonis⁴, Susan Harvey⁴, Mary Jane Cullen⁴, Hongwei Zhang⁵, Christian Caporuscio⁵, Paul Stetsko⁴, Mary Grubb⁴, Christine Huang⁴, Lisa Zhang⁴, Chris Freeden⁴, Brian J Murphy⁴, Jeffrey A Robl², William N Washburn²

Affiliations

¹ Metabolic Diseases Chemistry, Bristol-Myers Squibb Research and Development, Princeton, NJ 08543-5400, United States. Electronic address: [email protected].
² Metabolic Diseases Chemistry, Bristol-Myers Squibb Research and Development, Princeton, NJ 08543-5400, United States.
³ BMS-Biocon Research Center, Biocon, 20th KM, Hosur Road, Electronic City, Bangalore 560 100, India.
⁴ Metabolic Diseases Biology, Bristol-Myers Squibb Research and Development, Princeton, NJ 08543-5400, United States.
⁵ Pharmaceutical Candidate Optimization, Bristol-Myers Squibb Research and Development, Princeton, NJ 08543-5400, United States.

PMID: 26386604
DOI: 10.1016/j.bmcl.2015.09.018

Abstract

Non-basic azolotriazinones were explored using an empirical free brain exposures-driven approach to identify potent MCHR1 antagonists for evaluation in in vivo efficacy studies. An optimized lead from this series, 1j (rMCHR1 Ki=1.8 nM), demonstrated a 6.9% reduction in weight gain relative to vehicle in a rat model at 30 mg/kg after 4 days of once-daily oral treatment as a glycine prodrug. Despite a promising efficacy profile, an assessment of the biliary toxicity risk of this compound rendered this compound non-progressible.

Keywords: Anti-obesity; Biliary toxicity; Metabolite toxicity; Non-basic MCHR1 antagonists; Off-rates.

MeSH terms

Animals
Brain / drug effects*
Brain / metabolism
Dose-Response Relationship, Drug
Humans
Molecular Structure
Obesity / drug therapy*
Obesity / metabolism
Rats
Receptors, Somatostatin / antagonists & inhibitors*
Structure-Activity Relationship
Triazines / administration & dosage
Triazines / chemistry
Triazines / pharmacology*

Substances

MCHR1 protein, human
Receptors, Somatostatin
Triazines
azolotriazinone