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The role of interfacial lipids in stabilising membrane protein oligomers

Abstract:
Oligomerisation of membrane proteins in response to lipid binding plays a critical role in many cell-signaling pathways 1 but is often difficult to define 2 or predict 3. Here we develop a mass spectrometry platform to determine simultaneously presence of interfacial lipids and oligomeric stability and discover how lipids act as key regulators of membrane protein association. Evaluation of oligomeric strength for a dataset of 125 α-helical oligomeric membrane proteins revealed an absence of interfacial lipids in the mass spectra of 12 membrane proteins with high oligomeric stability. For the bacterial homologue of the eukaryotic biogenic transporters (LeuT) 4 one of the proteins with the lowest oligomeric stability, we found a precise cohort of lipids within the dimer interface. Delipidation, mutation of lipid binding sites or expression in cardiolipin (CDL) deficient Escherichia coli, abrogated dimer formation. Molecular dynamics simulation revealed that CDL acts as a bidentate ligand bridging across subunits. Subsequently, we show that for the sugar transporter SemiSWEET from Vibrio splendidus 5, another protein with low oligomeric stability, cardiolipin shifts the equilibrium from monomer to functional dimer. We hypothesised that lipids would be essential for dimerisation of the Na+/H+ antiporter NhaA from E. coli, which has the lowest oligomeric strength, but not for substantially more stable, homologous NapA from Thermus thermophilus. We found that lipid binding is obligatory for dimerisation of NhaA, whereas NapA has adapted to form an interface that is stable without lipids. Overall, by correlating interfacial strength with the presence of interfacial lipids we provide a rationale for understanding the role of lipids in both transient and stable interactions within a range of α-helical membrane proteins, including GPCRs.
Publication status:
Published
Peer review status:
Peer reviewed

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Publisher copy:
10.1038/nature20820

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Institution:
University of Oxford
Division:
MPLS
Department:
Chemistry
Sub department:
Physical & Theoretical Chem
Role:
Author
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Institution:
University of Oxford
Division:
MPLS
Department:
Chemistry
Sub department:
Physical & Theoretical Chem
Role:
Author
More by this author
Institution:
University of Oxford
Division:
MPLS
Department:
Chemistry
Sub department:
Physical & Theoretical Chem
Role:
Author
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Funding agency for:
Baldwin, A
Grant:
David Phillip’s Fellowship, BB/J014346/1
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Grant:
Advanced Grant ENABLE (641317)
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Grant:
Investigator Award (104633/Z/14/Z)
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Publisher:
Nature Publishing Group
Journal:
Nature More from this journal
Volume:
541
Issue:
7637
Pages:
421–424
Publication date:
2017-01-01
Acceptance date:
2016-11-14
DOI:
EISSN:
1476-4687
ISSN:
0028-0836

Pubs id:
pubs:664822
UUID:
uuid:9faf0660-9e0f-4983-b5f1-aab427f258e3
Local pid:
pubs:664822
Source identifiers:
664822
Deposit date:
2016-12-09

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