Stereoselective synthesis of erythro-3-fluorophenylalanine

v5+ -Catalyzed t-butylhydroperoxide epoxidation of (Z)-5-hydroxy-2- alkenylsilanes 4 exhibit good to excellent ervthro selectivity. The resulting epoxides undergo fragmentation to afford 1,3-diols 8, albeit in low chemical yield. Many natural products of current interest contain either a 1,3-diol s

Both diastereomers of racemic y-hydroxynorvaline were prepared from 4-penten-2-01 to illustrate a new general method for stereoselective synthesis of either eryrhro-or three-1,3-amino alcohol systems from a single precursor. Non-proteinogenic y-hydroxy-a-amino acids are an important class of natura

A concise and stereoselective synthesis of racemic erythro-methylphenidate (1) is described. The coupling reaction between piperidine-2-thione (3) and 2-bromo-2-phenylmethylacetate (4) afforded the b-enaminocarbonyl compound 2 in 60% yield by a modified Eschenmoser sulfide contraction reaction. In m

D-erythro-sphingosine and D-esythro-sphinganine can be produced in protected form from serine by a synthetic approach in which the normal biological intermediate 3-ketosphinganine in protectyed form, is a key synthetic intermediate. The sequence is short and convergent, proceeds in good overall yiel