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    J Biol Chem. 2010 Jan 22;285(4):2537-44. Epub 2009 Nov 16.

    The binding mode of ATP revealed by the solution structure of the N-domain of human ATP7A.

    Banci L, Bertini I, Cantini F, Inagaki S, Migliardi M, Rosato A.

    Source

    Magnetic Resonance Center (CERM) and Department of Chemistry, University of Florence, Italy.

    Abstract

    We report the solution NMR structures of the N-domain of the Menkes protein (ATP7A) in the ATP-free and ATP-bound forms. The structures consist of a twisted antiparallel six-stranded beta-sheet flanked by two pairs of alpha-helices. A protein loop of 50 amino acids located between beta 3 and beta 4 is disordered and mobile on the subnanosecond time scale. ATP binds with an affinity constant of (1.2 +/- 0.1) x 10(4) m(-1) and exchanges with a rate of the order of 1 x 10(3) s(-1). The ATP-binding cavity is considerably affected by the presence of the ligand, resulting in a more compact conformation in the ATP-bound than in the ATP-free form. This structural variation is due to the movement of the alpha1-alpha2 and beta2-beta 3 loops, both of which are highly conserved in copper(I)-transporting P(IB)-type ATPases. The present structure reveals a characteristic binding mode of ATP within the protein scaffold of the copper(I)-transporting P(IB)-type ATPases with respect to the other P-type ATPases. In particular, the binding cavity contains mainly hydrophobic aliphatic residues, which are involved in van der Waal's interactions with the adenine ring of ATP, and a Glu side chain, which forms a crucial hydrogen bond to the amino group of ATP.

    PMID:
    19917612
    [PubMed - indexed for MEDLINE]
    PMCID: PMC2807310
    Free PMC Article

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