Mishra, Saurabh ; Shukla, Prashant ; Bhaskar, Ashima ; Anand, Kushi ; Baloni, Priyanka ; Jha, Rajiv Kumar ; Mohan, Abhilash ; Rajmani, Raju S. ; Nagaraja, Valakunja ; Chandra, Nagasuma ; Singh, Amit (2017) Efficacy of β-lactam/β-lactamase inhibitor combination is linked to WhiB4-mediated changes in redox physiology of Mycobacterium tuberculosis elife, 6 . Article ID e25624. ISSN 2050-084X
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Official URL: https://elifesciences.org/articles/25624
Related URL: http://dx.doi.org/10.7554/eLife.25624
Abstract
Mycobacterium tuberculosis (Mtb) expresses a broad-spectrum β-lactamase (BlaC) that mediates resistance to one of the highly effective antibacterials, β-lactams. Nonetheless, β-lactams showed mycobactericidal activity in combination with β-lactamase inhibitor, clavulanate (Clav). However, the mechanistic aspects of how Mtb responds to β-lactams such as Amoxicillin in combination with Clav (referred as Augmentin [AG]) are not clear. Here, we identified cytoplasmic redox potential and intracellular redox sensor, WhiB4, as key determinants of mycobacterial resistance against AG. Using computer-based, biochemical, redox-biosensor, and genetic strategies, we uncovered a functional linkage between specific determinants of β-lactam resistance (e.g. β-lactamase) and redox potential in Mtb. We also describe the role of WhiB4 in coordinating the activity of β-lactamase in a redox-dependent manner to tolerate AG. Disruption of WhiB4 enhances AG tolerance, whereas overexpression potentiates AG activity against drug-resistant Mtb. Our findings suggest that AG can be exploited to diminish drug-resistance in Mtb through redox-based interventions.
Item Type: | Article |
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Source: | Copyright of this article belongs to eLife Sciences Publications. |
ID Code: | 112526 |
Deposited On: | 18 Apr 2018 11:49 |
Last Modified: | 18 Apr 2018 11:49 |
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