Review
General and specific lipid–protein interactions in Na,K-ATPase

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Highlights

  • General and specific interactions of lipids and Na,K-ATPase.

  • Specific lipid-binding sites in Na,K-ATPase E1 and E2 crystal structures.

  • Functional effects of specifically bound phospholipids and cholesterol on Na,K-ATPase activity.

  • Stimulatory, inhibitory and stabilizing effects of specifically bound lipids on Na,K-ATPase.

  • Bulk, annular and specifically bound lipids in Na,K-ATPase.

Abstract

The molecular activity of Na,K-ATPase and other P2 ATPases like Ca2 +-ATPase is influenced by the lipid environment via both general (physical) and specific (chemical) interactions. Whereas the general effects of bilayer structure on membrane protein function are fairly well described and understood, the importance of the specific interactions has only been realized within the last decade due particularly to the growing field of membrane protein crystallization, which has shed new light on the molecular details of specific lipid–protein interactions. It is a remarkable observation that specific lipid–protein interactions seem to be evolutionarily conserved, and conformations of specifically bound lipids at the lipid–protein surface within the membrane are similar in crystal structures determined with different techniques and sources of the protein, despite the rather weak lipid–protein interaction energy. Studies of purified detergent-soluble recombinant αβ or αβFXYD Na,K-ATPase complexes reveal three separate functional effects of phospholipids and cholesterol with characteristic structural selectivity. The observations suggest that these three effects are exerted at separate binding sites for phophatidylserine/cholesterol (stabilizing), polyunsaturated phosphatidylethanolamine (stimulatory), and saturated PC or sphingomyelin/cholesterol (inhibitory), which may be located within three lipid-binding pockets identified in recent crystal structures of Na,K-ATPase. The findings point to a central role of direct and specific interactions of different phospholipids and cholesterol in determining both stability and molecular activity of Na,K-ATPase and possible implications for physiological regulation by membrane lipid composition. This article is part of a special issue titled “Lipid–Protein Interactions.”

Abbreviations

CHL
cholesterol
C12E8
octaethylene glycol monodecyl ether
DDM
n-dodecyl-β-d-maltoside
DHA
decosahexaenoic acid
EP
phosphoenzyme
ld and lo
liquid-disordered and liquid-ordered phase
MD
molecular dynamic
nc
number of carbon atoms in lipid acyl chains
PC
phosphatidylcholine
PE
phosphatidylethanolamine
PI
phosphatidylinositol
PL
phospholipid
PS
phosphatidylserine
PSD
phosphatidyl serine decarboxylase
PUFA
polyunsaturated fatty acids
SERCA
sarco(endo)plasmic reticulum Ca-ATPase
SM
sphingomyelin
TM
transmembrane

Keywords

Na,K-ATPase phospholipid
Cholesterol
Reconstitution
Specific lipid–protein interactions
X-ray crystal structure
Recombinant Na,K-ATPase complexes

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This article is part of a Special Issue titled: Lipid–protein interactions.

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