Introducing of novel class of pyrano[2,3- c ]pyrazole-5-carbonitrile analogs with potent antimicrobial activity, DNA gyrase inhibition, and prominent pharmacokinetic and CNS toxicity profiles supported by molecular dynamic simulation.
Mohammed AlmaghrabiArafa MusaAhmed K B AljohaniHany E A AhmedMarwa AlsulaimanySamar F MiskiEhab M MostafaShaimaa HusseinDella Grace Thomas ParambiMohammed M GhoneimWalid E ElgammalAhmed H HalawaAli HammadAhmed M El-AgrodyPublished in: Journal of biomolecular structure & dynamics (2023)
Microbiological DNA gyrase is recognized as an exceptional microbial target for the innovative development of low-resistant and more effective antimicrobial drugs. Hence, we introduced a one-pot facile synthesis of a novel pyranopyrazole scaffold bearing different functionalities; substituted aryl ring, nitrile, and hydroxyl groups. All new analogs were characterized with full spectroscopic data. The antimicrobial screening for all analogs was assessed against standard strains of Gm + ve and Gm-ve through in vitro considers. The screened compounds displayed very promising MIC/MBC values against some of the bacterial strains with broad or selective antibacterial effects. Of these, 4j biphenyl analog showed 0.5-2/2-8 µ g/mL MIC/MBC for suppression and killing of Gm + ve and Gm-ve strains. Moreover, the antimicrobial screening was assessed for the most potent analogs against certain highly resistant microbial strains. Consequently, DNA gyrase supercoiling assay was done for all analogs using ciprofloxacin as reference positive control. Obviously, the results showed a different activity profile with potent analog 4j with IC 50 value 6.29 µ g/mL better than reference drug 10.2 µ g/mL. Additionally, CNS toxicity testing was done using the HiB5 cell line for attenuation of GABA/NMDA expression to both 4j and ciprofloxacin compounds that revealed better neurotransmitter modulation by novel scaffold. Importantly, docking and dynamic simulations were performed for the most active 4j analog to investigate its interaction with DNA binding sites, which supported the in vitro observations and compound stability with binding pocket. Finally, a novel scaffold pyranopyrazole was introduced as a DNA gyrase inhibitor with prominent antibacterial efficacy and low CNS side effect toxicity better than quinolones.Communicated by Ramaswamy H. Sarma.
Keyphrases
- molecular docking
- circulating tumor
- single molecule
- molecular dynamics simulations
- escherichia coli
- cell free
- staphylococcus aureus
- anti inflammatory
- oxidative stress
- microbial community
- blood brain barrier
- molecular dynamics
- pseudomonas aeruginosa
- nucleic acid
- tissue engineering
- poor prognosis
- circulating tumor cells
- silver nanoparticles
- big data
- electronic health record
- drug induced
- deep learning
- small molecule
- long non coding rna