4.5 Article

The evolution of A-, F-, and V-type ATP synthases and ATPascs:: reversals in function and changes in the H+/ATP coupling ratio

Journal

FEBS LETTERS
Volume 576, Issue 1-2, Pages 1-4

Publisher

WILEY-BLACKWELL
DOI: 10.1016/j.febslet.2004.08.065

Keywords

A(c)A(1); FoF1; VoV1; ATP synthase; ATPase

Funding

  1. NIGMS NIH HHS [GM23152] Funding Source: Medline

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Members of the F0F1, A(0)A(1) and V0V1 family of ATP synthases and ATPases have undergone at least two reversals in primary function. The first was from a progenitor proton-pumping ATPase to a proton-driven ATP synthase. The second involved transforming the synthase back into a proton-pumping ATPase. As proposed earlier [FEBS Lett. 259 (1990) 227], these reversals required changes in the H+/ATP coupling ratio from an optimal value of about 2 for an ATPase function to about 4 for an ATP synthase function. The doubling of the ratio that occurred at the ATPase-to-Synthase transition was accomplished by duplicating the gene that encodes the nucleotide-binding catalytic subunits followed by loss of function in one of the genes. The halving of the ratio that occurred at the Synthaseto-ATPase transition was achieved by a duplication/fusion of the gene that encodes the proton-binding transporter subunits, followed by a loss of function in one half of the double-sized protein. These events allowed conservation of quaternary structure, while maintaining a sufficient driving force to sustain an adequate phosphorylation potential or electrochemical gradient. Here, we describe intermediate evolutionary steps and a fine-tuning of the H+/ATP coupling ratio to optimize synthase function in response to different environments. In addition, we propose a third reversal of function, from an ATPase back to an ATP synthase. In contrast to the first two reversals which required a partial loss in function, the change in coupling ratio required for the third reversal is explained by a gain in function. (C) 2004 Federation of European Biochemical Societies. Published by Elsevier B.V. All rights reserved.

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