The First Large-Scale Synthesis of MK-4305: A Dual Orexin Receptor Antagonist for the Treatment of Sleep Disorder

Carl A. Baxter,Ed Cleator,Karel M. J. Brands,John S. Edwards,Robert A. Reamer,Faye J. Sheen,Gavin W. Stewart,Neil A. Strotman,Debra J. Wallace

The First Large-Scale Synthesis of MK-4305: A Dual Orexin Receptor Antagonist for the Treatment of Sleep Disorder

2011

Carl A. Baxter
Ed Cleator
Karel M. J. Brands
John S. Edwards
Robert A. Reamer
Faye J. Sheen
Gavin W. Stewart
Neil A. Strotman
Debra J. Wallace

A new synthetic route to drug candidate 1, a potent and selective dual orexin antagonist for the treatment of sleep disorders, has been developed. The key acyclic precursor 10 was prepared in a one-step process in 75% isolated yield from commercially available starting materials using novel chemistry to synthesize 2-substituted benzoxazoles. A reductive amination was followed by a classical resolution to afford chiral diazepane (R)-11. Finally, coupling of (R)-11 with acid 5 furnished the desired drug candidate 1.

Keywords:

Orexin antagonist
Orexin receptor
Reductive amination
Sleep disorder
Stereochemistry
Chemistry
Antagonist
Combinatorial chemistry
drug candidate
Chirality (chemistry)

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