Bimodal plasma metabolomics strategy identifies novel inflammatory metabolites in inflammatory bowel diseases

Yunki Y Yau; Rupert W L Leong; Sean Shin; Sonia Bustamante; Russell Pickford; Leila Hejazi; Beth Campbell; Valerie C Wasinger

Bimodal plasma metabolomics strategy identifies novel inflammatory metabolites in inflammatory bowel diseases

Discov Med. 2014 Sep;18(98):113-24.

Authors

Yunki Y Yau¹, Rupert W L Leong², Sean Shin³, Sonia Bustamante³, Russell Pickford³, Leila Hejazi³, Beth Campbell³, Valerie C Wasinger³

Affiliations

¹ Bioanalytical Mass Spectrometry Facility, Mark Wainwright Analytical Centre, The University of New South Wales, Kensington, NSW 2000, Australia and Department of Gastroenterology, Concord Repatriation General Hospital, Concord, NSW 2139, Australia.
² Department of Gastroenterology, Concord Repatriation General Hospital, Concord, NSW 2139, Australia and the Department of Gastroenterology, Bankstown-Lidcombe Hospital, Bankstown, NSW 2200, Australia.
³ Bioanalytical Mass Spectrometry Facility, Mark Wainwright Analytical Centre, The University of New South Wales, Kensington, NSW 2000, Australia.

PMID: 25227752

Abstract

Introduction: Crohn's disease (CD) and ulcerative colitis (UC) are inflammatory bowel diseases (IBD) characterized by variable phenotypes. Metabolites are signatures of biochemical activity that can reveal unknown pathogenic pathways. We employed untargeted mass spectrometry (MS) based metabolomics to identify novel inflammatory mechanisms in IBD and a targeted assay to quantify metabolites of the auto-immunomodulating kynurenine pathway (KP) in IBDs and health.

Materials and methods: Metabolome analysis of CD, UC, and control plasmas was performed on a Liquid Chromatography (LC)-MS/MS system. KP metabolites quinolinic acid (QA) and picolinic acid (PA) were quantified by gas chromatography/MS.

Results: Nineteen UC, 25 CD, and 9 control plasmas were analyzed: 34 metabolites exhibited abundance profiles associated with CD by global metabolome analysis (P≤0.05, false discovery rate q≤0.01). Notably, inflammatory-implicated metabolites angiotensin IV (P=0.049, q<0.001), diphthamide (P=0.018, q<0.001), and GM3 gangliosides (P<0.001, q<0.001) were increased in CD. By targeted kynurenine metabolites assay, QA (73.53 ng/mL ± 23.40 SD) and combined kynurenine metabolites (CKM) were increased in CD (120.19 ± 39.71) compared to controls (QA 50.14 ± 15.04; P<0.01; CKM 92.73 ± 26.30; P<0.01). CD QA positively correlated with CDAI (r=0.85; P<0.01), CRP (r=0.46; P=0.01), and ESR (r=0.42; P=0.03), while CKMs correlated with CDAI (r=0.615; P<0.01) and CRP (r=0.615; P=0.02).

Conclusions: Associations of angiotensin IV, diphthamide, and GM3 gangliosides with CD implicate novel pathways in activating a Th1/Th17 inflammatory profile. Increased QA concentrations in CD may indicate a defective auto-immunomodulation mechanism.

MeSH terms

Adult
Angiotensin II / analogs & derivatives
Angiotensin II / blood
Case-Control Studies
Colitis, Ulcerative / blood
Colitis, Ulcerative / immunology
Crohn Disease / blood
Crohn Disease / immunology
Female
G(M3) Ganglioside / blood
Histidine / analogs & derivatives
Histidine / blood
Humans
Inflammation Mediators / blood
Inflammatory Bowel Diseases / blood*
Inflammatory Bowel Diseases / immunology
Kynurenine / blood
Male
Metabolic Networks and Pathways
Metabolome*
Metabolomics
Middle Aged
Picolinic Acids / blood
Pilot Projects
Quinolinic Acid / blood
Tandem Mass Spectrometry
Young Adult

Substances

G(M3) Ganglioside
Inflammation Mediators
Picolinic Acids
Angiotensin II
angiotensin II, des-Asp(1)-des-Arg(2)-Ile(5)-
Kynurenine
Histidine
diphthamide
Quinolinic Acid
picolinic acid