Chemical Approach for Investigation of the Structure‐Activity Relationship of Salmycin and Identification of a Glycan‐based Analogue for Drug Resistant Staphylococcus aureus

Author:

Chiu Cheng‐Hsin1,Huang De‐Yi1,Ma Wei‐Hsiang1,Chen Yu‐Xun1,Yang Sih‐Yu1,Chen Yu‐Chie1,Tony Mong Kwok‐Kong1ORCID

Affiliation:

1. Applied Chemistry Department National Yang Ming Chiao Tung University (Previously National Chiao Tung University) 1001, University Road, Eastern District Hsinchu City 300093 Taiwan, ROC

Abstract

AbstractNew synthetic routes were devised for total synthesis of Fe3+‐bound (ferri−) salmycin B (Sal B) (1), glycan‐based Sal analogues 25 and their Fe3+‐unbound (desferri−) counterparts 1′5′ for the structure to activity relationship (SAR) study. The results of SAR study reveal the effective structure of 1 and its desferri‐counterpart 1′ that are responsible for the observed inhibitory activity against Staphylococcus aureus (S. aureus). Among the analogues 25 and 2′5′, glucose‐based analogue 2 and its desferri‐counterpart 2′ exhibited inhibitory potency comparable to 1 and 1′. Chemical modification of 2′ for further antibacterial study enabled us to discover desferri‐Sal analogue 7′ that endowed with a simpler pharmacophore structure but significantly higher antibacterial potency against methicillin‐sensitive and resistant S. aureus than the natural product 1′ and even the clinical vancomycin. Together with a better hydrolytic stability and shorter synthetic route, the analogue 7′ represents an attractive antibiotic lead for further exploration.

Funder

National Science and Technology Council

Publisher

Wiley

Subject

General Chemistry

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