Purification and membrane reconstitution of catalytically active Menkes copper-transporting P-type ATPase (MNK; ATP7A)

Hung, YH; Layton, MJ; Voskoboinik, I; Mercer, JFB; Camakaris, J

Author(s): Hung, YH; Layton, MJ; Voskoboinik, I; Mercer, JFB; Camakaris, J;
Journal Title: BIOCHEMICAL JOURNAL
Publication Type: Journal Article
Abstract: The MNK (Menkes disease protein; ATP7A) is a major copper-transporting P-type ATPase involved in the delivery of copper to cuproenzymes in the secretory pathway and the efflux of excess copper from extrahepatic tissues. Mutations in the MNK (ATP7A) gene result in Menkes disease, a fatal neurodegenerative copper deficiency disorder. Currently, detailed biochemical and biophysical analyses of MNK to better understand its mechanisms of copper transport are not possible due to the lack of purified MNK in an active form. To address this issue, we expressed human MNK with an N-terminal Glu-Glu tag in Sf9 [Spodoptera frugiperda (fall armyworm) 9] insect cells and purified it by antibody affinity chromatography followed by size-exclusion chromatography in the presence of the non-ionic detergent DDM (n-dodecyl beta-D-maltopyranoside). Formation of the classical vanadate-sensitive phosphoenzyme by purified MNK was activated by Cu(I) [EC50 = 0.7 mu M; h (Hill coefficient) was 4.6]. Furthermore, we report the first measurement of Cu(I)-dependent ATPase activity of MNK (K-0.5 = 0.6 mu M; h = 5.0). The purified MNK demonstrated active ATP-dependent vectorial Cu-64 transport when reconstituted into soya-bean asolectin liposomes. Together, these data demonstrated that Cu(I) interacts with MNK in a co-operative manner and with high affinity in the sub-micromolar range. The present study provides the first biochemical characterization of a purified full-length mammalian copper-transponing P-type ATPase associated with a human disease.
Publisher: PORTLAND PRESS LTD
Keywords: WILSONS-DISEASE PROTEIN; N-TERMINAL DOMAIN; LOW-COPY-NUMBER; ESCHERICHIA-COLI; CALCIUM-PUMP; SARCOPLASMIC-RETICULUM; CANDIDATE GENE; REGULATED TRAFFICKING; CELLULAR PHARMACOLOGY; NH2-TERMINAL DOMAIN
Publisher's Version: https://doi.org/10.1042/BJ20060924
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Creation Date: 2007-01-15 12:00:00