Staphylococcus aureus responds to allicin by global S-thioallylation - Role of the Brx/BSH/YpdA pathway and the disulfide reductase MerA to overcome allicin stress.
Loi VV, Huyen NTT, Busche T, Tung QN, Gruhlke MCH, Kalinowski J, Bernhardt J, Slusarenko AJ, Antelmann H (2019)
Free radical biology & medicine 139: 55-69.
Zeitschriftenaufsatz
| Veröffentlicht | Englisch
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Autor*in
Loi, Vu Van;
Huyen, Nguyen Thi Thu;
Busche, TobiasUniBi;
Tung, Quach Ngoc;
Gruhlke, Martin Clemens Horst;
Kalinowski, JörnUniBi;
Bernhardt, Jorg;
Slusarenko, Alan John;
Antelmann, Haike
Einrichtung
Abstract / Bemerkung
The prevalence of methicillin-resitant Staphylococcus aureus (MRSA) in hospitals and the community poses an increasing health burden, which requires the discovery of alternative antimicrobials. Allicin (diallyl thiosulfinate) from garlic exhibits broad-spectrum antimicrobial activity against many multidrug resistant bacteria. The thiol-reactive mode of action of allicin involves its S-thioallylations of low molecular weight (LMW) thiols and protein thiols. To investigate the mode of action and stress response caused by allicin in S. aureus, we analyzed the transcriptome signature, the targets for S-thioallylation in the proteome and the changes in the bacillithiol (BSH) redox potential (EBSH) under allicin stress. Allicin caused a strong thiol-specific oxidative and sulfur stress response and protein damage as revealed by the induction of the PerR, HypR, QsrR, MhqR, CstR, CtsR, HrcA and CymR regulons in the RNA-seq transcriptome. Allicin also interfered with metal and cell wall homeostasis and caused induction of the Zur, CsoR and GraRS regulons. Brx-roGFP2 biosensor measurements revealed a strongly increased EBSH under allicin stress. In the proteome, 57 proteins were identified with S-thioallylations under allicin treatment, including translation factors (EF-Tu, EF-Ts), metabolic and redox enzymes (AldA, GuaB, Tpx, KatA, BrxA, MsrB) as well as redox-sensitive MarR/SarA-family regulators (MgrA, SarA, SarH1, SarS). Phenotype and biochemical analyses revealed that BSH and the HypR-controlled disulfide reductase MerA are involved in allicin detoxification in S. aureus. The reversal of protein S-thioallylation was catalyzed by the Brx/BSH/YpdA pathway. Finally, the BSSB reductase YpdA was shown to use S-allylmercaptobacillithiol (BSSA) as substrate to regenerate BSH in S. aureus. In conclusion, allicin results in an oxidative shift of EBSH and protein S-thioallylation, which can be reversed by YpdA and the Brx/BSH/YpdA electron pathways in S. aureus to regenerate thiol homeostasis. Copyright © 2019 The Authors. Published by Elsevier Inc. All rights reserved.
Erscheinungsjahr
2019
Zeitschriftentitel
Free radical biology & medicine
Band
139
Seite(n)
55-69
ISSN
1873-4596
Page URI
https://pub.uni-bielefeld.de/record/2935892
Zitieren
Loi VV, Huyen NTT, Busche T, et al. Staphylococcus aureus responds to allicin by global S-thioallylation - Role of the Brx/BSH/YpdA pathway and the disulfide reductase MerA to overcome allicin stress. Free radical biology & medicine. 2019;139:55-69.
Loi, V. V., Huyen, N. T. T., Busche, T., Tung, Q. N., Gruhlke, M. C. H., Kalinowski, J., Bernhardt, J., et al. (2019). Staphylococcus aureus responds to allicin by global S-thioallylation - Role of the Brx/BSH/YpdA pathway and the disulfide reductase MerA to overcome allicin stress. Free radical biology & medicine, 139, 55-69. doi:10.1016/j.freeradbiomed.2019.05.018
Loi, Vu Van, Huyen, Nguyen Thi Thu, Busche, Tobias, Tung, Quach Ngoc, Gruhlke, Martin Clemens Horst, Kalinowski, Jörn, Bernhardt, Jorg, Slusarenko, Alan John, and Antelmann, Haike. 2019. “Staphylococcus aureus responds to allicin by global S-thioallylation - Role of the Brx/BSH/YpdA pathway and the disulfide reductase MerA to overcome allicin stress.”. Free radical biology & medicine 139: 55-69.
Loi, V. V., Huyen, N. T. T., Busche, T., Tung, Q. N., Gruhlke, M. C. H., Kalinowski, J., Bernhardt, J., Slusarenko, A. J., and Antelmann, H. (2019). Staphylococcus aureus responds to allicin by global S-thioallylation - Role of the Brx/BSH/YpdA pathway and the disulfide reductase MerA to overcome allicin stress. Free radical biology & medicine 139, 55-69.
Loi, V.V., et al., 2019. Staphylococcus aureus responds to allicin by global S-thioallylation - Role of the Brx/BSH/YpdA pathway and the disulfide reductase MerA to overcome allicin stress. Free radical biology & medicine, 139, p 55-69.
V.V. Loi, et al., “Staphylococcus aureus responds to allicin by global S-thioallylation - Role of the Brx/BSH/YpdA pathway and the disulfide reductase MerA to overcome allicin stress.”, Free radical biology & medicine, vol. 139, 2019, pp. 55-69.
Loi, V.V., Huyen, N.T.T., Busche, T., Tung, Q.N., Gruhlke, M.C.H., Kalinowski, J., Bernhardt, J., Slusarenko, A.J., Antelmann, H.: Staphylococcus aureus responds to allicin by global S-thioallylation - Role of the Brx/BSH/YpdA pathway and the disulfide reductase MerA to overcome allicin stress. Free radical biology & medicine. 139, 55-69 (2019).
Loi, Vu Van, Huyen, Nguyen Thi Thu, Busche, Tobias, Tung, Quach Ngoc, Gruhlke, Martin Clemens Horst, Kalinowski, Jörn, Bernhardt, Jorg, Slusarenko, Alan John, and Antelmann, Haike. “Staphylococcus aureus responds to allicin by global S-thioallylation - Role of the Brx/BSH/YpdA pathway and the disulfide reductase MerA to overcome allicin stress.”. Free radical biology & medicine 139 (2019): 55-69.
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