Phospholipid Profiling Established by Structure‐Rich Fragments for Molecular Species Level Shotgun Analysis
Rong Chen, Amber H. Jannasch, Bruce R. Cooper, Jonathan H. Shannahan, Christina R. Ferreira

TL;DR
This study introduces a new method for accurately identifying phospholipid species in lipidomics, improving biomarker discovery for metabolic diseases.
Contribution
A novel MRM-based approach using structure-rich fragments for high-throughput, specific phospholipid identification in shotgun lipidomics.
Findings
15 PUFA-containing phospholipids were identified as biomarkers in mouse livers with metabolic syndrome.
Three ether lipid biomarkers were discovered in mouse brains, including plasmalogens and plasmanyl lipids.
Structure-rich MS/MS transitions improved phospholipid specificity while maintaining high throughput.
Abstract
Accurate identification of phospholipid molecular species remains a major challenge in shotgun lipidomics because conventional tandem mass spectrometry typically resolves only one structural moiety at a time. This structural ambiguity limits confident lipid biomarker discovery and biological interpretation. Improving structural specificity without sacrificing analytical speed is therefore critical for lipidomics and disease‐related studies. Electrospray ionization tandem mass spectrometry was performed using direct infusion on a triple quadrupole mass spectrometer operated in multiple reaction monitoring (MRM) mode. MRMs were designed based on structure‐rich phospholipid fragments containing both the headgroup and one fatty acyl chain. Lipids were extracted from mouse liver and brain tissues and analysed without chromatographic separation, and normal‐phase LC was used for lipid…
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Taxonomy
TopicsMetabolomics and Mass Spectrometry Studies · Mass Spectrometry Techniques and Applications · Fatty Acid Research and Health
