Targeting multidrug resistant Staphylococcus aureus with cationic chlorpromazine‐peptide conjugates

Author:

Panjla Apurva1,Kaul Grace23,Akhir Abdul4,Saxena Deepanshi2,Joshi Saurabh1,Modak Chandrima5,Kumari Dipti5,Jain Alok5,Chopra Sidharth23,Verma Sandeep14

Affiliation:

1. Department of Chemistry Indian Institute of Technology Kanpur Kanpur 208016 UP India

2. Department of Molecular Microbiology and Immunology CSIR-Central Drug Research Institute, Sector 10 Sitapur Road, Janakipuram Extension Lucknow 226031 UP India

3. AcSIR: Academy of Scientific and Innovative Research (AcSIR) Ghaziabad 201002 India

4. Mehta Family Center for Engineering in Medicine Center for Nanoscience Indian Institute of Technology Kanpur Kanpur 208016 UP India

5. Department of Bioengineering and Biotechnology Birla Institute of Technology Mesra Ranchi 835215 Jharkhand India

Abstract

AbstractAntimicrobial resistance is a serious public health risk. Its severity is fueled on an unprecedented scale, necessitating the demand for novel antimicrobial scaffolds aimed at novel targets. Herein, we present cationic chlorpromazine peptide conjugates that are rationally intended to targetmultidrug‐resistant (MDR) bacteria. The most potent compound, CPWL, of all the conjugates evaluated, showed promising antibacterial activity against clinical, MDR S. aureus, with no cytotoxicity. The molecular docking experiments confirmed that CPWL possessed a very high affinity for S. aureus enoyl reductase (saFabI). Furthermore, CPWL antibacterial action against saFabI was further corroborated by MD simulation studies. Thus, our findings highlight cationic chlorpromazine as a promising scaffold for the development of saFabI inhibitors to target severe staphylococcal infections.

Publisher

Wiley

Subject

General Chemistry,Biochemistry,Organic Chemistry

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