Repositioning of Disulfiram in Association with Vancomycin Against Enterococcus spp. MDR and XDR
Marissa B. Serafin
1
,
Vitória S. Foletto
1
,
Taciéli F Da Rosa
1
,
Angelita Bottega
1
,
Altevir Rossato Viana
2
,
Laísa Nunes Franco
3
,
Sara De Lima Marion
1
,
Augusto Dias Da Mota
1
,
Bruno Rafael De Paula
3
,
Luciana Maria Fontanari Krause
3
,
Luis Junior Finatto
4
,
Manfredo Hörner
5
,
Rosmari Hörner
1, 3
4
Hospital Universitário de Santa Maria, Santa Maria, Brazil
|
Publication type: Journal Article
Publication date: 2022-03-18
scimago Q2
wos Q3
SJR: 0.621
CiteScore: 4.8
Impact factor: 2.6
ISSN: 03438651, 14320991
PubMed ID:
35303186
General Medicine
Microbiology
Applied Microbiology and Biotechnology
Abstract
The identification of molecules that exhibit potent antibacterial activity and are capable of circumventing resistance mechanisms is an unmet need. The repositioning of approved drugs is considered an advantageous alternative in this case, and has gained prominence. In addition, drug synergism can reduce morbidity and mortality in the treatment of nosocomial infections caused by multi-drug resistant microorganisms (MDR). Whole cell growth inhibition assays were used to define the in vitro antibacterial activity of disulfiram against two standard American Type Culture Collection (ATCC) strains and 35 clinical isolates of vancomycin-resistant enterococci (VRE). The ability of disulfiram to synergize with vancomycin was determined by fractional inhibitory concentration index, preceded by the checkerboard test. The cytotoxicity of drugs alone and in combination was tested against Raw 264.7 cells. Disulfiram exhibited potent antibacterial activity against VRE (MIC 16–64 µg mL−1). Results: Associated with vancomycin, disulfiram it had a reduction in MIC of up to 64 times, with values of 0.5–4 µg mL−1. Vancomycin had a MIC of 128–1024 µg mL−1; combined, reduced this value by up to 124 times (8 µg mL−1), with synergy occurring against all strains. Disulfiram and vancomycin alone and in combination did not show cytotoxicity against the eukaryotic cell line. Based on these results, we suggest that the redirection of disulfiram may be promising in the treatment of infections caused by VRE, since it was able to potentiate the activity of vancomycin against the strains, being able to act as an adjuvant in cases of serious infections caused by Enterococcus.
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Total citations:
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Citations from 2024:
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(60%)
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Serafin M. B. et al. Repositioning of Disulfiram in Association with Vancomycin Against Enterococcus spp. MDR and XDR // Current Microbiology. 2022. Vol. 79. No. 5. 137
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Serafin M. B., Foletto V. S., Da Rosa T. F., Bottega A., Viana A. R., Franco L. N., De Lima Marion S., Da Mota A. D., De Paula B. R., Krause L. M. F., Finatto L. J., Hörner M., Hörner R. Repositioning of Disulfiram in Association with Vancomycin Against Enterococcus spp. MDR and XDR // Current Microbiology. 2022. Vol. 79. No. 5. 137
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TY - JOUR
DO - 10.1007/s00284-022-02794-9
UR - https://doi.org/10.1007/s00284-022-02794-9
TI - Repositioning of Disulfiram in Association with Vancomycin Against Enterococcus spp. MDR and XDR
T2 - Current Microbiology
AU - Serafin, Marissa B.
AU - Foletto, Vitória S.
AU - Da Rosa, Taciéli F
AU - Bottega, Angelita
AU - Viana, Altevir Rossato
AU - Franco, Laísa Nunes
AU - De Lima Marion, Sara
AU - Da Mota, Augusto Dias
AU - De Paula, Bruno Rafael
AU - Krause, Luciana Maria Fontanari
AU - Finatto, Luis Junior
AU - Hörner, Manfredo
AU - Hörner, Rosmari
PY - 2022
DA - 2022/03/18
PB - Springer Nature
IS - 5
VL - 79
PMID - 35303186
SN - 0343-8651
SN - 1432-0991
ER -
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BibTex (up to 50 authors)
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@article{2022_Serafin,
author = {Marissa B. Serafin and Vitória S. Foletto and Taciéli F Da Rosa and Angelita Bottega and Altevir Rossato Viana and Laísa Nunes Franco and Sara De Lima Marion and Augusto Dias Da Mota and Bruno Rafael De Paula and Luciana Maria Fontanari Krause and Luis Junior Finatto and Manfredo Hörner and Rosmari Hörner},
title = {Repositioning of Disulfiram in Association with Vancomycin Against Enterococcus spp. MDR and XDR},
journal = {Current Microbiology},
year = {2022},
volume = {79},
publisher = {Springer Nature},
month = {mar},
url = {https://doi.org/10.1007/s00284-022-02794-9},
number = {5},
pages = {137},
doi = {10.1007/s00284-022-02794-9}
}