Comparison of conformation and antimicrobial activity of synthetic analogs of gramicidin S: Stereochemical consideration of the role of D ‐phenylalanine in the antibiotic

In order to study the role of D ‐amino acid residues in keeping the stable β‐sheet conformation and in the antimicrobial activity of gramicidin S (GS), the four analogs of GS containing D ‐Ala, L ‐Ala, Gly, and Aib (α‐aminoisobutyric acid) in place of D ‐Phe were synthesized. D ‐Ala‐and Gly‐containing analogs showed antimicrobial activity, while those containing L ‐Ala and Aib showed no activity. Conformation of these analogs and their derivatives were studied by comparison of ORD and CD spectra and by slective methylation method. It is concluded that the biologically active analogs have β‐sheet conformation while inactive analogs have a much different conformation from that of GS. This indicates that D ‐Ala‐Pro and Gly‐Pro sequences favor taking a β‐bend form but L ‐Ala‐Pro and Aib‐Pro sequences do not because the presence of L ‐side methyl group on the α‐carbon atom of L Ala and Aib residues destabilizes the β‐bend form. This would explain why the inactive analogs which take a different conformation from that of the active ones result in the loss of activity.