Article

Validation of membrane protein topology models by oxidative labeling and mass spectrometry.

Department of Chemistry, The University of Western Ontario, London, Ontario, N6A 5B7, Canada.
Journal of the American Society for Mass Spectrometry (impact factor: 4). 03/2012; 23(5):889-98. DOI:10.1007/s13361-012-0342-x pp.889-98
Source: PubMed

ABSTRACT Computer-assisted topology predictions are widely used to build low-resolution structural models of integral membrane proteins (IMPs). Experimental validation of these models by traditional methods is labor intensive and requires modifications that might alter the IMP native conformation. This work employs oxidative labeling coupled with mass spectrometry (MS) as a validation tool for computer-generated topology models. ·OH exposure introduces oxidative modifications in solvent-accessible regions, whereas buried segments (e.g., transmembrane helices) are non-oxidizable. The Escherichia coli protein WaaL (O-antigen ligase) is predicted to have 12 transmembrane helices and a large extramembrane domain (Pérez et al., Mol. Microbiol. 2008, 70, 1424). Tryptic digestion and LC-MS/MS were used to map the oxidative labeling behavior of WaaL. Met and Cys exhibit high intrinsic reactivities with ·OH, making them sensitive probes for solvent accessibility assays. Overall, the oxidation pattern of these residues is consistent with the originally proposed WaaL topology. One residue (M151), however, undergoes partial oxidation despite being predicted to reside within a transmembrane helix. Using an improved computer algorithm, a slightly modified topology model was generated that places M151 closer to the membrane interface. On the basis of the labeling data, it is concluded that the refined model more accurately reflects the actual topology of WaaL. We propose that the combination of oxidative labeling and MS represents a useful strategy for assessing the accuracy of IMP topology predictions, supplementing data obtained in traditional biochemical assays. In the future, it might be possible to incorporate oxidative labeling data directly as constraints in topology prediction algorithms.

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Keywords

12 transmembrane helices
 
actual topology
 
computer-generated topology models
 
Escherichia coli protein WaaL
 
Experimental validation
 
improved computer algorithm
 
integral membrane proteins
 
labeling data
 
low-resolution structural models
 
modified topology model
 
oxidative labeling data
 
proposed WaaL topology
 
refined model
 
sensitive probes
 
supplementing data
 
topology prediction algorithms
 
traditional biochemical assays
 
transmembrane helix
 
Tryptic digestion
 
undergoes partial oxidation
 

Yan Pan