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J Org Chem
July 1996
Department of Chemical Research, Sphinx Pharmaceuticals, A Division of Eli Lilly and Company, 4615 University Drive, Durham, North Carolina 27707.
Two total syntheses of the potent protein kinase C inhibitory fungal metabolite balanol are described. In the first approach, the core aminohydroxyazepane subunit was prepared in racemic form by stereospecific functionalization of N-benzyl-epsilon-caprolactam. Resolution prior to coupling to the benzophenone subunit provided access to both enantiomers of balanol.
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