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Novel antibiofilm chemotherapies target nitrogen from glutamate and glutamine.


ABSTRACT: Bacteria in nature often reside in differentiated communities termed biofilms, which are an active interphase between uni-cellular and multicellular life states for bacteria. Here we demonstrate that the development of B. subtilis biofilms is dependent on the use of glutamine or glutamate as a nitrogen source. We show a differential metabolic requirement within the biofilm; while glutamine is necessary for the dividing cells at the edges, the inner cell mass utilizes lactic acid. Our results indicate that biofilm cells preserve a short-term memory of glutamate metabolism. Finally, we establish that drugs that target glutamine and glutamate utilization restrict biofilm development. Overall, our work reveals a spatial regulation of nitrogen and carbon metabolism within the biofilm, which contributes to the fitness of bacterial complex communities. This acquired metabolic division of labor within biofilm can serve as a target for novel anti-biofilm chemotherapies.

SUBMITTER: Hassanov T 

PROVIDER: S-EPMC5940852 | biostudies-literature | 2018 May

REPOSITORIES: biostudies-literature

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Novel antibiofilm chemotherapies target nitrogen from glutamate and glutamine.

Hassanov Tal T   Karunker Iris I   Steinberg Nitai N   Erez Ayelet A   Kolodkin-Gal Ilana I  

Scientific reports 20180508 1


Bacteria in nature often reside in differentiated communities termed biofilms, which are an active interphase between uni-cellular and multicellular life states for bacteria. Here we demonstrate that the development of B. subtilis biofilms is dependent on the use of glutamine or glutamate as a nitrogen source. We show a differential metabolic requirement within the biofilm; while glutamine is necessary for the dividing cells at the edges, the inner cell mass utilizes lactic acid. Our results ind  ...[more]

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