Role of post-translational modifications at the β-subunit ectodomain in complex association with a promiscuous plant P4-ATPase

P-type ATPases of subfamily IV (P4-ATPases) constitute a major group of phospholipid flippases that form heteromeric complexes with members of the Cdc50 (cell division control 50) protein family. Some P4-ATPases interact specifically with only one β-subunit isoform, whereas others are promiscuous an...

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Published inBiochemical journal Vol. 473; no. 11; p. 1605
Main Authors Costa, Sara R, Marek, Magdalena, Axelsen, Kristian B, Theorin, Lisa, Pomorski, Thomas G, López-Marqués, Rosa L
Format Journal Article
LanguageEnglish
Published England 01.06.2016
Subjects
Adenosine Triphosphatases - chemistry
Adenosine Triphosphatases - genetics
Adenosine Triphosphatases - metabolism
Asparagine - chemistry
Asparagine - genetics
Asparagine - metabolism
Cysteine - chemistry
Cysteine - genetics
Cysteine - metabolism
Mutation
Nicotiana - metabolism
Plant Proteins - chemistry
Plant Proteins - genetics
Plant Proteins - metabolism
Plants, Genetically Modified - genetics
Plants, Genetically Modified - metabolism
Protein Binding
Protein Domains - genetics
Protein Domains - physiology
Protein Processing, Post-Translational
Protein Subunits - chemistry
Protein Subunits - genetics
Protein Subunits - metabolism
Protein Transport - genetics
Protein Transport - physiology
Arabidopsis thaliana
disulfide bond
flippase
Cdc50 ectodomain
N-glycosylation
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Summary:P-type ATPases of subfamily IV (P4-ATPases) constitute a major group of phospholipid flippases that form heteromeric complexes with members of the Cdc50 (cell division control 50) protein family. Some P4-ATPases interact specifically with only one β-subunit isoform, whereas others are promiscuous and can interact with several isoforms. In the present study, we used a site-directed mutagenesis approach to assess the role of post-translational modifications at the plant ALIS5 β-subunit ectodomain in the functionality of the promiscuous plant P4-ATPase ALA2. We identified two N-glycosylated residues, Asn(181) and Asn(231) Whereas mutation of Asn(231) seems to have a small effect on P4-ATPase complex formation, mutation of evolutionarily conserved Asn(181) disrupts interaction between the two subunits. Of the four cysteine residues located in the ALIS5 ectodomain, mutation of Cys(86) and Cys(107) compromises complex association, but the mutant β-subunits still promote complex trafficking and activity to some extent. In contrast, disruption of a conserved disulfide bond between Cys(158) and Cys(172) has no effect on the P4-ATPase complex. Our results demonstrate that post-translational modifications in the β-subunit have different functional roles in different organisms, which may be related to the promiscuity of the P4-ATPase.
ISSN:1470-8728
DOI:10.1042/BCJ20160207