Literature DB >> 28265968

Expanding Lipidome Coverage Using LC-MS/MS Data-Dependent Acquisition with Automated Exclusion List Generation.

Jeremy P Koelmel1, Nicholas M Kroeger2, Emily L Gill1, Candice Z Ulmer1,3, John A Bowden3, Rainey E Patterson1, Richard A Yost1,4, Timothy J Garrett5,6.   

Abstract

Untargeted omics analyses aim to comprehensively characterize biomolecules within a biological system. Changes in the presence or quantity of these biomolecules can indicate important biological perturbations, such as those caused by disease. With current technological advancements, the entire genome can now be sequenced; however, in the burgeoning fields of lipidomics, only a subset of lipids can be identified. The recent emergence of high resolution tandem mass spectrometry (HR-MS/MS), in combination with ultra-high performance liquid chromatography, has resulted in an increased coverage of the lipidome. Nevertheless, identifications from MS/MS are generally limited by the number of precursors that can be selected for fragmentation during chromatographic elution. Therefore, we developed the software IE-Omics to automate iterative exclusion (IE), where selected precursors using data-dependent topN analyses are excluded in sequential injections. In each sequential injection, unique precursors are fragmented until HR-MS/MS spectra of all ions above a user-defined intensity threshold are acquired. IE-Omics was applied to lipidomic analyses in Red Cross plasma and substantia nigra tissue. Coverage of the lipidome was drastically improved using IE. When applying IE-Omics to Red Cross plasma and substantia nigra lipid extracts in positive ion mode, 69% and 40% more molecular identifications were obtained, respectively. In addition, applying IE-Omics to a lipidomics workflow increased the coverage of trace species, including odd-chained and short-chained diacylglycerides and oxidized lipid species. By increasing the coverage of the lipidome, applying IE to a lipidomics workflow increases the probability of finding biomarkers and provides additional information for determining etiology of disease. Graphical Abstract ᅟ.

Entities:  

Keywords:  Data-dependent Analysis; Diglyceride; Lipidomics; Lipids; Mass spectrometry; Metabolomics; Tandem mass spectrometry

Year:  2017        PMID: 28265968      PMCID: PMC5408749          DOI: 10.1007/s13361-017-1608-0

Source DB:  PubMed          Journal:  J Am Soc Mass Spectrom        ISSN: 1044-0305            Impact factor:   3.109


  32 in total

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  37 in total

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Authors:  Jeremy P Koelmel; Candice Z Ulmer; Christina M Jones; Richard A Yost; John A Bowden
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2.  Chronic maternal cortisol excess during late gestation leads to metabolic alterations in the newborn heart.

Authors:  Jacquelyn M Walejko; Andrew Antolic; Jeremy P Koelmel; Timothy J Garrett; Arthur S Edison; Maureen Keller-Wood
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3.  Metabolomic and lipidomic characterization of Oxalobacter formigenes strains HC1 and OxWR by UHPLC-HRMS.

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4.  Lipidomics for wildlife disease etiology and biomarker discovery: a case study of pansteatitis outbreak in South Africa.

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5.  A Robust Lipidomics Workflow for Mammalian Cells, Plasma, and Tissue Using Liquid-Chromatography High-Resolution Tandem Mass Spectrometry.

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9.  Multiomics approach reveals metabolic changes in the heart at birth.

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10.  Pioglitazone improves hepatic mitochondrial function in a mouse model of nonalcoholic steatohepatitis.

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