Structure Activity Relationship Studies on Rhodanines and Derived Enethiol Inhibitors of Metallo-β-Lactamases
Bioorganic and Medicinal Chemistry 2018
D. Zhang, M.S. Markoulides, Dmitrijs Stepanovs, A.M. Rydzik, A. El-Hussein, C. Bon, J.J.A.G. Kamps, K.-D. Umland, P.M. Collins, S.T. Cahill, D.Y. Wang, F. von Delft, J. Brem, M.A. Mcdonough, C.J. Schofield

Metallo-β-lactamases (MBLs) enable bacterial resistance to almost all classes of β-lactam antibiotics. We report studies on enethiol containing MBL inhibitors, which were prepared by rhodanine hydrolysis. The enethiols inhibit MBLs from different subclasses. Crystallographic analyses reveal that the enethiol sulphur displaces the di-Zn(II) ion bridging ‘hydrolytic’ water. In some, but not all, cases biophysical analyses provide evidence that rhodanine/enethiol inhibition involves formation of a ternary MBL enethiol rhodanine complex. The results demonstrate how low molecular weight active site Zn(II) chelating compounds can inhibit a range of clinically relevant MBLs and provide additional evidence for the potential of rhodanines to be hydrolysed to potent inhibitors of MBL protein fold and, maybe, other metallo-enzymes, perhaps contributing to the complex biological effects of rhodanines. The results imply that any medicinal chemistry studies employing rhodanines (and related scaffolds) as inhibitors should as a matter of course include testing of their hydrolysis products.


Keywords
Antibiotic resistance, Carbapenemase, Inhibitors, Metallo β-lactamase, Structure activity relationships
DOI
10.1016/j.bmc.2018.02.043
Hyperlink
https://www.ncbi.nlm.nih.gov/pubmed/29655609

Zhang, D., Markoulides, M., Stepanovs, D., Rydzik, A., El-Hussein, A., Bon, C., Kamps, J., Umland, K., Collins, P., Cahill, S., Wang, D., von Delft, F., Brem, J., Mcdonough, M., Schofield, C. Structure Activity Relationship Studies on Rhodanines and Derived Enethiol Inhibitors of Metallo-β-Lactamases. Bioorganic and Medicinal Chemistry, 2018, Vol.26, No.11, pp.2928-2936. ISSN 0968-0896. Available from: doi:10.1016/j.bmc.2018.02.043

Publication language
English (en)
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