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Conserved inter-domain interactions drive trans-Golgi network localisation and trafficking of homologous copper-ATPases
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Abstract
Polytopic transmembrane Copper-ATPases are central regulators of the essential, redox-active micronutrient copper in all organisms. The vertebrate Cu-ATPase homologs ATP7A and ATP7B facilitate excess copper efflux, in addition to metalating cuproproteins. ATP7A and ATP7B exhibit copper-responsive basolateral and apical trafficking polarity respectively, in polarized epithelia. To elucidate the role of conserved functional domains in copper-responsive trafficking and copper transport, we substituted the copper-binding amino-terminal, Nucleotide-Binding (NBD) and C-terminal domain of ATP7B with that of ATP7A either singly or in combinations. The six chimeric Cu-ATPases generated, although functionally active, exhibited altered trafficking phenotypes. Notably, the N-terminal-substituted ATP7B exhibited constitutive trafficking to the basolateral membrane; however, the N-terminal and NBD double-substituted chimera gained steady-state TGN localization, indicating a putative interaction between the two domains critical for its TGN-localization. We analyzed orthologous Cu-ATPase domain sequences from diverse organisms and found that the N-terminal domain and NBD showed similar evolutionary relationships, unlike that of C-terminal domain, suggesting their co-evolution. This study for the first time correlates evolutionary stringency imparted onto Cu-ATPase domains with their significance in proper trafficking regulation.
Title: Conserved inter-domain interactions drive trans-Golgi network localisation and trafficking of homologous copper-ATPases
Description:
Abstract
Polytopic transmembrane Copper-ATPases are central regulators of the essential, redox-active micronutrient copper in all organisms.
The vertebrate Cu-ATPase homologs ATP7A and ATP7B facilitate excess copper efflux, in addition to metalating cuproproteins.
ATP7A and ATP7B exhibit copper-responsive basolateral and apical trafficking polarity respectively, in polarized epithelia.
To elucidate the role of conserved functional domains in copper-responsive trafficking and copper transport, we substituted the copper-binding amino-terminal, Nucleotide-Binding (NBD) and C-terminal domain of ATP7B with that of ATP7A either singly or in combinations.
The six chimeric Cu-ATPases generated, although functionally active, exhibited altered trafficking phenotypes.
Notably, the N-terminal-substituted ATP7B exhibited constitutive trafficking to the basolateral membrane; however, the N-terminal and NBD double-substituted chimera gained steady-state TGN localization, indicating a putative interaction between the two domains critical for its TGN-localization.
We analyzed orthologous Cu-ATPase domain sequences from diverse organisms and found that the N-terminal domain and NBD showed similar evolutionary relationships, unlike that of C-terminal domain, suggesting their co-evolution.
This study for the first time correlates evolutionary stringency imparted onto Cu-ATPase domains with their significance in proper trafficking regulation.
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