Literature DB >> 29595093

Synergy of clavine alkaloid 'chanoclavine' with tetracycline against multi-drug-resistant E. coli.

Gaurav Raj Dwivedi1,2, Anupam Maurya3,4, Dharmendra Kumar Yadav5,6, Vigyasa Singh1, Feroz Khan5, Mahendra Kumar Gupta7, Mastan Singh7, Mahendra P Darokar1, Santosh Kumar Srivastava3.   

Abstract

The emergence of multi drug resistance (MDR) in Gram-negative bacteria (GNB) and lack of novel classes of antibacterial agents have raised an immediate need to identify antibacterial agents, which can reverse the phenomenon of MDR. The purpose of present study was to evaluate synergy potential and understanding the drug resistance reversal mechanism of chanoclavine isolated from Ipomoea muricata against the multi-drug-resistant clinical isolate of Escherichia coli (MDREC). Although chanoclavine did not show antibacterial activity of its own, but in combination, it could reduce the minimum inhibitory concentration (MIC) of tetracycline (TET) up to 16-folds. Chanoclavine was found to inhibit the efflux pumps which seem to be ATPase-dependent. In real-time expression analysis, chanoclavine showed down-regulation of different efflux pump genes and decreased the mutation prevention concentration of tetracycline. Further, in silico docking studies revealed significant binding affinity of chanoclavine with different proteins known to be involved in drug resistance. In in silico ADME/toxicity studies, chanoclavine was found safe with good intestinal absorption, aqueous solubility, medium blood-brain barrier (BBB), no CYP 2D6 inhibition, no hepatotoxicity, no skin irritancy, and non-mutagenic indicating towards drug likeliness of this molecule. Based on these observations, it is hypothesized that chanoclavine might be inhibiting the efflux of tetracycline from MDREC and thus enabling the more availability of tetracycline inside the cell for its action.

Entities:  

Keywords:  ADMET; antibacterial combinations; chanoclavine; efflux pump inhibitor; multi-drug-resistant (MDREC)

Mesh:

Substances:

Year:  2018        PMID: 29595093     DOI: 10.1080/07391102.2018.1458654

Source DB:  PubMed          Journal:  J Biomol Struct Dyn        ISSN: 0739-1102


  10 in total

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  10 in total

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