Solution Structure of the Transmembrane H+-transporting Subunit C of the F1F0 ATP Synthase

Overview

Journal Biochemistry

Specialty Biochemistry

Date 1998 Jun 24

PMID 9636021

Citations 82

Authors

M E Girvin

V K Rastogi

F Abildgaard

J L Markley

R H Fillingame

Affiliations

Soon will be listed here.

Abstract

Subunit c is the H+-translocating component of the F1F0 ATP synthase complex. H+ transport is coupled to conformational changes that ultimately lead to ATP synthesis by the enzyme. The properties of the monomeric subunit in a single-phase solution of chloroform-methanol-water (4:4:1) have been shown to mimic those of the protein in the native complex. Triple resonance NMR experiments were used to determine the complete structure of monomeric subunit c in this solvent mixture. The structure of the protein was defined by >2000 interproton distances, 64 (3)JN alpha, and 43 hydrogen-bonding NMR-derived restraints. The root mean squared deviation for the backbone atoms of the two transmembrane helices was 0.63 A. The protein folds as a hairpin of two antiparallel helical segments, connected by a short structured loop. The conserved Arg41-Gln42-Pro43 form the top of this loop. The essential H+-transporting Asp61 residue is located at a slight break in the middle of the C-terminal helix, just prior to Pro64. The C-terminal helix changes direction by 30 +/- 5 degrees at the conserved Pro64. In its protonated form, the Asp61 lies in a cavity created by the absence of side chains at Gly23 and Gly27 in the N-terminal helix. The shape and charge distribution of the molecular surface of the monomeric protein suggest a packing arrangement for the oligomeric protein in the F0 complex, with the front face of one monomer packing favorably against the back face of a second monomer. The packing suggests that the proton (cation) binding site lies between packed pairs of adjacent subunit c.

Citing Articles

Rotational Mechanism of F Motor in the F-Type ATP Synthase Driven by the Proton Motive Force.

Kubo S, Takada S Front Microbiol. 2022; 13:872565.

PMID: 35783438 PMC: 9243769. DOI: 10.3389/fmicb.2022.872565.

Rotor subunits adaptations in ATP synthases from photosynthetic organisms.

Cheuk A, Meier T Biochem Soc Trans. 2021; 49(2):541-550.

PMID: 33890627 PMC: 8106487. DOI: 10.1042/BST20190936.

Solution NMR: A powerful tool for structural and functional studies of membrane proteins in reconstituted environments.

Puthenveetil R, Vinogradova O J Biol Chem. 2019; 294(44):15914-15931.

PMID: 31551353 PMC: 6827292. DOI: 10.1074/jbc.REV119.009178.

Structural Asymmetry and Kinetic Limping of Single Rotary F-ATP Synthases.

Sielaff H, Yanagisawa S, Frasch W, Junge W, Borsch M Molecules. 2019; 24(3).

PMID: 30704145 PMC: 6384691. DOI: 10.3390/molecules24030504.

Antibacterial isoamphipathic oligomers highlight the importance of multimeric lipid aggregation for antibacterial potency.

Brown J, Mohamed Z, Artim C, Thornlow D, Hassler J, Rigoglioso V Commun Biol. 2018; 1:220.

PMID: 30534612 PMC: 6286309. DOI: 10.1038/s42003-018-0230-4.