Asymmetric Synthesis of Highly Functionalized Tetrahydropyran DPP‑4 Inhibitor

Asymmetric Synthesis of Highly Functionalized Tetrahydropyran DPP‑4 Inhibitor

A practical synthesis of a highly functionalized tetrahydropyran DPP-4 inhibitor is described. The asymmetric synthesis relies on three back-to-back Ru-catalyzed reactions. A Ru-catalyzed dynamic kinetic resolution (DKR) reduction establishes two contiguous stereogenic centers in one operation. A un...

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Veröffentlicht in:Organic letters 2014-10, Vol.16 (20), p.5422-5425
Hauptverfasser: Xu, Feng, Zacuto, Michael J, Kohmura, Yoshinori, Rosen, Jon, Gibb, Andrew, Alam, Mahbub, Scott, Jeremy, Tschaen, David
Format: Artikel
Sprache:eng
Schlagworte:
Amination
Catalysis
Dipeptidyl-Peptidase IV Inhibitors - chemical synthesis
Dipeptidyl-Peptidase IV Inhibitors - chemistry
Dipeptidyl-Peptidase IV Inhibitors - pharmacology
Enzyme Inhibitors
Glycine - analogs & derivatives
Glycine - chemistry
Hypoglycemic Agents
Kinetics
Molecular Structure
Oxidation-Reduction
Pyrones - chemical synthesis
Pyrones - chemistry
Pyrones - pharmacology
Ruthenium - chemistry
Stereoisomerism
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Zusammenfassung:A practical synthesis of a highly functionalized tetrahydropyran DPP-4 inhibitor is described. The asymmetric synthesis relies on three back-to-back Ru-catalyzed reactions. A Ru-catalyzed dynamic kinetic resolution (DKR) reduction establishes two contiguous stereogenic centers in one operation. A unique dihydropyran ring is efficiently constructed through a preferred Ru-catalyzed cycloisomerization. Hydroboration followed by a Ru-catalyzed oxidation affords the desired functionalized pyranone core scaffold. Finally, stereoselective reductive amination and subsequent acidic deprotection afford the desired, potent DPP-4 inhibitor in 25% overall yield.
ISSN:1523-7060
1523-7052
DOI:10.1021/ol502661g