Total synthesis of Resolvin E1

Total synthesis of Resolvin E1

The enantioselective total synthesis of Resolvin E1 (RvE1), a naturally occurring small molecule mediator of inflammation resolution, is reported. Two routes are presented, both modular and convergent in nature, with an excellent control of all stereocenters. The C12- and C18-hydroxy groups are deri...

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Veröffentlicht in:Tetrahedron letters 2011-05, Vol.52 (21), p.2623-2626
Hauptverfasser: Allard, Melissa, Barnes, Keith, Chen, Xuemei, Cheung, Yiu-Yin, Duffy, Bryan, Heap, Charles, Inthavongsay, John, Johnson, Matthew, Krishnamoorthy, Ravi, Manley, Chris, Steffke, Stephan, Varughese, Deepu, Wang, Ruifang, Wang, Yi, Schwartz, C.E.
Format: Artikel
Sprache:eng
Schlagworte:
Aliphatic compounds
Chemistry
Disengaging
Enantioselective synthesis
Exact sciences and technology
Inflammation resolution
Ketones
Modular
Organic chemistry
Precursors
Preparations and properties
Reduction
Resolvin E1
Synthesis (chemistry)
Takai and Sonogashira couplings
Tetrahedrons
Total synthesis
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Zusammenfassung:The enantioselective total synthesis of Resolvin E1 (RvE1), a naturally occurring small molecule mediator of inflammation resolution, is reported. Two routes are presented, both modular and convergent in nature, with an excellent control of all stereocenters. The C12- and C18-hydroxy groups are derived from (S)-glycidol while the C5-hydroxy group is installed via enantioselective reduction of a ketone precursor. Both the cis-alkenes are introduced with excellent control by the reduction of a late-stage bis-alkyne intermediate. The synthetic disconnections are very amenable to analog preparation, and further modifications to the chemistry have allowed for scale-up and First in Man testing of this novel pro-resolution molecule.
ISSN:0040-4039
1873-3581
DOI:10.1016/j.tetlet.2011.03.035