First Stereocontrolled Synthesis of the (3 S ,5 R ,7 R ,10 R ,11 R )-C1−C13 Fragment of Nystatin A 1

## Abstract The ^13^C‐labelled putative erythromycin biosynthetic intermediates, ((2__S__,3__S__,4__S__,5__R__,6__R__,7__R__)‐3,6,7‐trihydroxy‐2,4,6‐trimethyl[1‐^13^C]nonan‐5‐olide and __S__‐2‐acetylaminoethyl (2__R__,3__S__,4__S__,5__R__,6__S__,7__R__)‐3,5,6,7‐tetrahydroxy‐2,4,6‐trimethyl[1‐^13^C]

## Abstract An efficient ^13^C‐labelling synthesis of the putative erythromycin biosynthetic intermediate, __S__‐2‐acetylaminoethyl (2__R__,3__R__,4__R__,5__R__)‐3,5‐diacetoxy‐2,4‐dimethyl‐4‐([^13^C]methoxy)heptanethioate, which would be useful for the investigation of the chain elongation mechanis

C-3 took place to some extent. The crude 2 was oxidized under the Swern condition to give (2S,3IZ,l'R)-stegobinone 1 in 14.0 % yield from 3 after purification by prep TLC. The unwanted by-product, (2S,3S,l'R)-stegobinone, could be removed by TLC separation. The IR and mass spectral properties of our

2-Ethoxy-1-methyl-5-pymlidinone (1) was reacted with ethyl [3,4-'3C2]acetoacetate (2) in the presence of T i c 4 to give ethyl [3,4-13C2]-2-( 1'-methyl-5'oxo-2'-pyrrolidinyl)-3-oxobutanoate (3) in 85% yield. Decarboethoxylation of ethyl [3,4-13C2]-2-( l'-methyl-5'-oxo-2'-pyrrolidiny1)-3-oxobutanoate