Synthesis of an Enantiomerically Pure Serine-Derived Thiazole

Synthesis of an Enantiomerically Pure Serine-Derived Thiazole. -The bulky trityl group is shown to be the N-protecting group of choice in the synthesis of serine-derived thiazole amino acids. The trityl-group serves as a protecting group in the key-step, the conversion of thioamide (V) to the thiaz

## Abstract L‐Tryptophan methyl ester reacts with 1,1,3,3‐tetramethoxypropane to give methyl carbolinecarboxylate 2 as a 1:2 mixture of the (1__R__,3__S__) and (1__S__,3__S__) stereoisomers. Conversion to the corresponding amides (1__R__,3__S__)‐3 and (1__S__,3__S__)‐3 was accomplished by treatment

The synthesis of enontiomericully pure mycQnosiio/ derivatives is accomplished using a mandeiic acid&rived acy/ protecting group. A number of synthetic schemes leading to enantiomerieally pure, and properly functionalized derivatives of myo-inositol start from one of the three positional isomers of

## Abstract An efficient stereocontrolled synthesis of (__S__)‐__N__‐Cbz‐serine (Cbz = benzyloxycarbonyl; 12) and of its (__R__)‐enantiomer is reported. Kinetic resolution of the easily available racemic 3‐(hydroxymethyl)‐1,4‐benzodiazepin‐2‐ones is performed in the key step __via__ acetylation by