At the heart of central carbon metabolism, pyruvate is a pivotal metabolite in all living cells. is able to excrete pyruvate as well as to use it as the sole carbon source. We herein reveal that (renamed ), the only operon specifically induced in pyruvate-grown cells, encodes a hetero-oligomeric membrane complex which operates as a facilitated transport system specific for pyruvate, thereby defining a novel class of transporter. We demonstrate that the LytST two-component system is responsible for the induction of in the presence of pyruvate by binding of the LytT response regulator to a palindromic region upstream of We show that both glucose and malate, the preferred carbon sources for , trigger the binding of CcpA upstream of , which results in its catabolite repression. However, an additional CcpA-independent mechanism represses in the presence of malate. Screening a genome-wide transposon mutant library, we find that an active malic enzyme replenishing the pyruvate pool is required for this repression. We next reveal that the higher the influx of pyruvate, the stronger the CcpA-independent repression of , which suggests that intracellular pyruvate retroinhibits induction via LytST. Such a retroinhibition challenges the rational design of novel nature-inspired sensors and synthetic switches but undoubtedly offers new possibilities for the development of integrated sensor/controller circuitry. Overall, we provide evidence for a complete system of sensors, feed-forward and feedback controllers that play a major role in environmental growth of Pyruvate is a small-molecule metabolite ubiquitous in living cells. Several species also use it as a carbon source as well as excrete it into the environment. The bacterial systems for pyruvate import/export have yet to be discovered. Here, we identified in the model bacterium the first import/export system specific for pyruvate, PftAB, which defines a novel class of transporter. In this bacterium, extracellular pyruvate acts as the signal molecule for the LytST two-component system (TCS), which in turn induces expression of PftAB. However, when the pyruvate influx is high, LytST activity is drastically retroinhibited. Such a retroinhibition challenges the rational design of novel nature-inspired sensors and synthetic switches but undoubtedly offers new possibilities for the development of integrated sensor/controller circuitry.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5626966PMC
http://dx.doi.org/10.1128/mBio.00976-17DOI Listing

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