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Quantitative profiling of bile acids in biofluids and tissues based on accurate mass high resolution LC-FT-MS: Compound class targeting in a metabolomics workflow

Authors :
Andreas P. Freidig
Elwin Verheij
Ivana Bobeldijk
R. Kleemann
Maarten Hekman
Teake Kooistra
Raymond Ramaker
Carina M. Rubingh
Leon Coulier
Jitske de Vries-van der Weij
TNO Kwaliteit van Leven
Source :
Journal of Chromatography B: Analytical Technologies in the Biomedical and Life Sciences, 2, 871, 306-313
Publication Year :
2008
Publisher :
Elsevier BV, 2008.

Abstract

We report a sensitive, generic method for quantitative profiling of bile acids and other endogenous metabolites in small quantities of various biological fluids and tissues. The method is based on a straightforward sample preparation, separation by reversed-phase high performance liquid-chromatography mass spectrometry (HPLC-MS) and electrospray ionisation in the negative ionisation mode (ESI-). Detection is performed in full scan using the linear ion trap Fourier transform mass spectrometer (LTQ-FTMS) generating data for many (endogenous) metabolites, not only bile acids. A validation of the method in urine, plasma and liver was performed for 17 bile acids including their taurine, sulfate and glycine conjugates. The method is linear in the 0.01-1 μM range. The accuracy in human plasma ranges from 74 to 113%, in human urine 77 to 104% and in mouse liver 79 to 140%. The precision ranges from 2 to 20% for pooled samples even in studies with large number of samples (n > 250). The method was successfully applied to a multi-compartmental APOE*3-Leiden mouse study, the main goal of which was to analyze the effect of increasing dietary cholesterol concentrations on hepatic cholesterol homeostasis and bile acid synthesis. Serum and liver samples from different treatment groups were profiled with the new method. Statistically significant differences between the diet groups were observed regarding total as well as individual bile acid concentrations. © 2008 Elsevier B.V. All rights reserved.

Subjects

Subjects :
Ionization
Metabolite
Biochemistry
High-performance liquid chromatography
Mass Spectrometry
Analytical Chemistry
Mice
Liquid chromatography–mass spectrometry
Bile acid synthesis
Cholesterol homeostasis
Homeostasis
Quantitative analysis
Accuracy
Liquid phase epitaxy
Spectrometers
Fourier Analysis
General Medicine
Chlorine compounds
Fourier transforms
HPLC-MS
Tissues
Cholesterol
Sulfate minerals
Complexation
Fourier Transform Mass Spectrometer
Human
Chromatography-mass spectrometry
Liquid chromatography
Phase separation
Glycine
Targeted metabolite profiling
Electro spraying
Mass spectrometry
Sample preparations
Article
Separation
Metabolomics
Generic methods
Humans
Animal experiment
Mouse liver
Analytical research
Cholesterol liver level
Tissue
Chromatography
Spectrometry
Computational Biology
Bile acids
Fourier transform mass spectrometry
chemistry
Acids
Taurine
Clinical Biochemistry
Animal tissue
Cholesterol, Dietary
chemistry.chemical_compound
Metabolites
Human urine
Priority journal
Linear ion trap
Bile acid
High resolutions
Human plasmas
Statistical significance
Body fluids
Liver
Biological fluids
Mass spectrometers
Histology
medicine.drug_class
Electrospray ionization
Reversed phase high performance liquid chromatography
Cholesterol intake
Bile Acids and Salts
Arsenic compounds
medicine
Animals
Reversed-phase high performance
Chromatographic analysis
Reproducibility of Results
Cell Biology
Electrospray
Nonhuman
Sulfate
Accurate mass
Metabolism
Plasmas
Bio-fluids
Pooled samples
Ionization of liquids
Body fluid
Controlled study
High performance liquid chromatography
Chromatography, Liquid

Details

ISSN :
15700232
Volume :
871
Database :
OpenAIRE
Journal :
Journal of Chromatography B
Accession number :
edsair.doi.dedup.....f0d80c443e23cbe780014c845b89da1e
Full Text :
https://doi.org/10.1016/j.jchromb.2008.05.008