Author/Authors :
Allard، نويسنده , , Melissa and Barnes، نويسنده , , Keith and Chen، نويسنده , , Xuemei and Cheung، نويسنده , , Yiu-Yin and Duffy، نويسنده , , Bryan and Heap، نويسنده , , Charles and Inthavongsay، نويسنده , , John and Johnson، نويسنده , , Matthew and Krishnamoorthy، نويسنده , , Ravi and Manley، نويسنده , , Chris and Steffke، نويسنده , , Stephan and Varughese، نويسنده , , Deepu and Wang، نويسنده , , Ruifang an، نويسنده ,
Abstract :
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.
Keywords :
Inflammation resolution , total synthesis , enantioselective synthesis , Takai and Sonogashira couplings , Resolvin E1
