In vitro potentiation of carbapenems with tannic acid against carbapenemase‐producing enterobacteriaceae : exploring natural products as potential carbapenemase inhibitors

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dc.contributor.author Somboro, A.M.
dc.contributor.author Osei Sekyere, John
dc.contributor.author Amoako, Daniel G.
dc.contributor.author Kumalo, Hezekiel M.
dc.contributor.author Khan, R.
dc.contributor.author Bester, L.A.
dc.contributor.author Essack, S.Y.
dc.date.accessioned 2019-01-11T07:35:43Z
dc.date.issued 2019-02
dc.description.abstract AIMS : We hypothesized and confirmed that tannic acid (TA) reverses carbapenem resistance by inhibiting carbapenemases in class A and B carbapenemase‐producing Enterobacteriaceae. METHODS AND RESULTS: Minimum inhibitory concentrations of carbapenems in the presence and absence of TA and other efflux pump inhibitors, TA‐carbapenemases inhibition assays and computational studies showed that TA had the greatest effect on metallo‐β‐lactamases (MBLs) followed by class A serine‐β‐lactamases (SBLs). TA completely reversed the MICs of MBL producers from between 32 and ≥512 mg l−1 to susceptible values (<4 mg l−1) while substantially reducing the MICs of SBLs from between 16 and >512 mg l−1 to <4 to 16 mg l−1. Tolerable cytotoxic effect was observed for the concentrations tested (8–1024 mg l−1). TA inhibited enzymes with a marked difference of ≈50% inhibition (IC50) for NDM‐1 (270 μmol l−1) and KPC‐2 (15 μmol l−1). CONCLUSION : TA inhibited both MBLs and SBLs by targeting their hydrophobic sites. Moreover, TA had a stronger binding affinity for MBLs than SBLs as the MBLs, specifically VIM‐1 (−43·7220 ± 0·4513 kcal mol−1) and NDM‐1(−44·2329 ± 0·3806 kcal mol−1), interact with a larger number of their catalytic active‐site residues than that of OXA‐48 (−22·5275 ± 0·1300 kcal mol−1) and KPC‐2 (−22·1164 ± 0·0111 kcal mol−1). SIGNIFICANCE AND IMPACT OF THE STUDY : Tannic acid or its analogues could be developed into carbapenemase‐inhibiting adjuvants to restore carbapenem activity in CRE infections, save many lives and reduce healthcare associated costs. en_ZA
dc.description.department Medical Microbiology en_ZA
dc.description.embargo 2020-02-01
dc.description.librarian hj2019 en_ZA
dc.description.sponsorship College of Health Sciences, University of Kwa‐Zulu Natal, Durban, South Africa and the South African National Research Foundation (NRF). en_ZA
dc.description.uri http://onlinelibrary.wiley.com/journal/10.1111/(ISSN)1365-2672 en_ZA
dc.identifier.citation Somboro, A.M., Osei Sekyere, J., Amoako, D.G. et al. 2018, 'In vitro potentiation of carbapenems with tannic acid against carbapenemase-producing enterobacteriaceae : exploring natural products as potential carbapenemase inhibitors', Journal of Applied Microbiology, vol. 126, no. 2, pp. 452-467. en_ZA
dc.identifier.issn 1364-5072 (print)
dc.identifier.issn 1365-2672 (online)
dc.identifier.other 10.1111/jam.14141
dc.identifier.uri http://hdl.handle.net/2263/68126
dc.language.iso en en_ZA
dc.publisher Wiley en_ZA
dc.rights © 2018 The Society for Applied Microbiology. This is the pre-peer reviewed version of the following article : 'In vitro potentiation of carbapenems with tannic acid against carbapenemase-producing enterobacteriaceae : exploring natural products as potential carbapenemase inhibitors', Journal of Applied Microbiology, vol. 126, no. 2, pp. 452-467, 2019, doi : 10.1111/jam.14141. The definite version is available at : http://onlinelibrary.wiley.comjournal/10.1111/(ISSN)1365-2672. en_ZA
dc.subject Tannic acid (TA) en_ZA
dc.subject Natural products en_ZA
dc.subject Carbapenem; en_ZA
dc.subject Carbapenemase en_ZA
dc.subject Efflux pump en_ZA
dc.subject Efflux pump inhibitors en_ZA
dc.subject Enterobacteriaceae en_ZA
dc.subject Enzymatic inhibition assay en_ZA
dc.subject Serine‐β‐lactamases (SBLs) en_ZA
dc.subject Metallo‐β‐lactamases (MBLs) en_ZA
dc.subject MBL inhibitors en_ZA
dc.title In vitro potentiation of carbapenems with tannic acid against carbapenemase‐producing enterobacteriaceae : exploring natural products as potential carbapenemase inhibitors en_ZA
dc.type Postprint Article en_ZA


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