1. Academic Validation
  2. Target identification, and optimization of dioxygenated amide derivatives as potent antibacterial agents with FabH inhibitory activity

Target identification, and optimization of dioxygenated amide derivatives as potent antibacterial agents with FabH inhibitory activity

  • Eur J Med Chem. 2023 Dec 16:265:116064. doi: 10.1016/j.ejmech.2023.116064.
Haoyun Chang 1 Ruiying Ji 2 Zhiyu Zhu 2 Yapin Wang 2 Shaopeng Yan 2 Dan He 2 Qike Jia 2 Peng Huang 3 Tao Cheng 4 Rui Wang 5 Yang Zhou 6
Affiliations

Affiliations

  • 1 School of Pharmacy, Anhui University of Chinese Medicine, Hefei, 230012, China; Cixi Institute of Biomedical Engineering, Ningbo Institute of Materials Technology and Engineering, Chinese Academy of Sciences, Ningbo, 315300, China.
  • 2 Cixi Institute of Biomedical Engineering, Ningbo Institute of Materials Technology and Engineering, Chinese Academy of Sciences, Ningbo, 315300, China.
  • 3 School of Pharmacy, Anhui University of Chinese Medicine, Hefei, 230012, China. Electronic address: great7701@ahtcm.edu.cn.
  • 4 Pharmaron (Ningbo) Technology Development Co. Ltd., Ningbo, 315336, China.
  • 5 Pingshan Translational Medicine Center, Shenzhen Bay Laboratory, Shenzhen, 518118, China. Electronic address: wangrui@szbl.ac.cn.
  • 6 Cixi Institute of Biomedical Engineering, Ningbo Institute of Materials Technology and Engineering, Chinese Academy of Sciences, Ningbo, 315300, China. Electronic address: zhouyang876@nimte.ac.cn.
Abstract

The Enzyme FabH plays a critical role in the initial step of fatty acid biosynthesis, which is vital for the survival of bacteria. As a result, FabH has emerged as an appealing target for the development of novel Antibacterial agents. In this study, employing the chemical proteomics method, we validated the previously identified skeleton amide derivatives bearing dioxygenated rings, potentially formed through metabolic processes. Building upon the proteomics findings, we then synthesized and evaluated 32 compounds containing N-heterocyclic amides for their antimicrobial activity for future optimizing the deoxygenated amides. Several compounds demonstrated potent antimicrobial properties with low toxicity, particularly compound 25, which exhibited remarkable potential as an agent with an MIC range of 1.25-3.13 μg/mL against the tested Bacterial strains and an IC50 of 2.0 μM against E. coli-derived FabH. Furthermore, we evaluated nine analogues with relatively low MIC values through cytotoxicity and hemolytic activity assessments, Lipinski's rule-of-five criteria, and in silico ADMET predictions to ascertain their druggability potential. Notably, a detailed docking simulation was performed to investigate the binding interactions of compound 25 within the binding pocket of E. coli FabH, which encouragingly revealed strong binding interactions. Based on our findings, compound 25 emerges as the optimal candidate for in vivo therapy aimed at treating infected skin defects. Remarkably, the application of compound 25 demonstrated a significant reduction in the duration of wound Infection and notably accelerated the healing process of infected wounds, achieving an impressive 94 % healing rate by day 10.

Keywords

Antibacterial-agent; Dioxygenated-amide derivatives; FabH inhibitor; Quantitative ABPP-based chemoproteomic identification.

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