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  4. Fluorescent Benzothiazinone Analogues Efficiently and Selectively Label Dpre1 in Mycobacteria and Actinobacteria
 
research article

Fluorescent Benzothiazinone Analogues Efficiently and Selectively Label Dpre1 in Mycobacteria and Actinobacteria

Sommer, Raphael  
•
Neres, Joao  
•
Piton, Jeremie  
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November 1, 2018
ACS Chemical Biology

Benzothiazinones (BTZ) are highly potent bactericidal inhibitors of mycobacteria and the lead compound, BTZ043, and the optimized drug candidate, PBTZ169, have potential for the treatment of tuberculosis. Here, we exploited the tractability of the BTZ scaffold by attaching a range of fluorophores to the 2-substituent of the BTZ ring via short linkers. We show by means of fluorescence imaging that the most advanced derivative, JN108, is capable of efficiently labeling its target, the essential flavoenzyme DprE1, both in cell-free extracts and after purification as well as in growing cells of different actinobacterial species. DprE1 displays a polar localization in Mycobacterium tuberculosis, M. marinum, M. smegmatis, and Nocardia farcinica but not in Corynebacterium glutamicum. Finally, mutation of the cysteine residue in DprE1 in these species, to which BTZ covalently binds, abolishes completely the interaction with JN108, thereby highlighting the specificity of this fluorescent probe.

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Type
research article
DOI
10.1021/acschembio.8b00790
Web of Science ID

WOS:000451100800018

Author(s)
Sommer, Raphael  
Neres, Joao  
Piton, Jeremie  
Dhar, Neeraj  
van der Sar, Astrid
Mukherjee, Raju  
Laroche, Thierry  
Dyson, Paul J.  
McKinney, John D.  
Bitter, Wilbert
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Date Issued

2018-11-01

Published in
ACS Chemical Biology
Volume

13

Issue

11

Start page

3184

End page

3192

Subjects

Biochemistry & Molecular Biology

•

drug discovery

•

tuberculosis

•

inhibitors

•

arabinan

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

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Available on Infoscience
December 13, 2018
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/152080
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