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A new type of Na(+)-driven ATP synthase membrane rotor with a two-carboxylate ion-coupling motif.


ABSTRACT: The anaerobic bacterium Fusobacterium nucleatum uses glutamate decarboxylation to generate a transmembrane gradient of Na?. Here, we demonstrate that this ion-motive force is directly coupled to ATP synthesis, via an F?F?-ATP synthase with a novel Na? recognition motif, shared by other human pathogens. Molecular modeling and free-energy simulations of the rotary element of the enzyme, the c-ring, indicate Na? specificity in physiological settings. Consistently, activity measurements showed Na? stimulation of the enzyme, either membrane-embedded or isolated, and ATP synthesis was sensitive to the Na? ionophore monensin. Furthermore, Na? has a protective effect against inhibitors targeting the ion-binding sites, both in the complete ATP synthase and the isolated c-ring. Definitive evidence of Na? coupling is provided by two identical crystal structures of the c?? ring, solved by X-ray crystallography at 2.2 and 2.6 Å resolution, at pH 5.3 and 8.7, respectively. Na? ions occupy all binding sites, each coordinated by four amino acids and a water molecule. Intriguingly, two carboxylates instead of one mediate ion binding. Simulations and experiments demonstrate that this motif implies that a proton is concurrently bound to all sites, although Na? alone drives the rotary mechanism. The structure thus reveals a new mode of ion coupling in ATP synthases and provides a basis for drug-design efforts against this opportunistic pathogen.

SUBMITTER: Schulz S 

PROVIDER: S-EPMC3692424 | biostudies-literature | 2013

REPOSITORIES: biostudies-literature

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A new type of Na(+)-driven ATP synthase membrane rotor with a two-carboxylate ion-coupling motif.

Schulz Sarah S   Iglesias-Cans Marina M   Krah Alexander A   Yildiz Ozkan O   Leone Vanessa V   Matthies Doreen D   Cook Gregory M GM   Faraldo-Gómez José D JD   Meier Thomas T  

PLoS biology 20130625 6


The anaerobic bacterium Fusobacterium nucleatum uses glutamate decarboxylation to generate a transmembrane gradient of Na⁺. Here, we demonstrate that this ion-motive force is directly coupled to ATP synthesis, via an F₁F₀-ATP synthase with a novel Na⁺ recognition motif, shared by other human pathogens. Molecular modeling and free-energy simulations of the rotary element of the enzyme, the c-ring, indicate Na⁺ specificity in physiological settings. Consistently, activity measurements showed Na⁺ s  ...[more]

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