Combining native and 'omics' mass spectrometry to identify endogenous ligands bound to membrane proteins

Agasid, M; Bolla, JR; Gault, J; Goodwin, M; Huguet, R; Jefferies, D; Khalid, S; Ladds, MJGW; Landreh, M; Lane, DP; Liko, I; McAlister, G; Mullen, C; Remes, PM; Robinson, CV; Shutinm, D; Syka, JEP; Viner, R; Yen, H-Y

Combining native and 'omics' mass spectrometry to identify endogenous ligands bound to membrane proteins

Authors: M Agasid
JR Bolla
J Gault
M Goodwin
R Huguet
D Jefferies
S Khalid
MJGW Ladds
M Landreh
DP Lane
I Liko
G McAlister
C Mullen
PM Remes
CV Robinson
D Shutinm
JEP Syka
R Viner
H-Y Yen
Publication date: 1 January 2020
Publisher: Springer Nature

Abstract

Ligands bound to protein assemblies provide critical information for function, yet are often difficult to capture and define. Here we develop a top-down method, 'nativeomics', unifying 'omics' (lipidomics, proteomics, metabolomics) analysis with native mass spectrometry to identify ligands bound to membrane protein assemblies. By maintaining the link between proteins and ligands, we define the lipidome/metabolome in contact with membrane porins and a mitochondrial translocator to discover potential regulators of protein function

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