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MALDI imaging MS reveals candidate lipid markers of polycystic kidney disease
Authors:Hermelindis Ruh  Theresia Salonikios  Jens Fuchser  Matthias Schwartz  Carsten Sticht  Christina Hochheim  Bernhard Wirnitzer  Norbert Gretz  Carsten Hopf
Institution:2. Center for Applied Research in Biomedical Mass Spectrometry (ABIMAS), and Mannheim University of Applied Sciences, 68163 Mannheim, Germany;11. Institute of Digital Signal Processing, Mannheim University of Applied Sciences, 68163 Mannheim, Germany;4. Institute of Medical Technology, University of Heidelberg and Mannheim University of Applied Sciences, 68167 Mannheim, Germany;8. Medical Research Center, Bruker Daltonik GmbH, D-28359 Bremen, Germany
Abstract:Autosomal recessive polycystic kidney disease (ARPKD) is a severe, monogenetically inherited kidney and liver disease. PCK rats carrying the orthologous mutant gene serve as a model of human disease, and alterations in lipid profiles in PCK rats suggest that defined subsets of lipids may be useful as molecular disease markers. Whereas MALDI protein imaging mass spectrometry (IMS) has become a promising tool for disease classification, widely applicable workflows that link MALDI lipid imaging and identification as well as structural characterization of candidate disease-classifying marker lipids are lacking. Here, we combine selective MALDI imaging of sulfated kidney lipids and Fisher discriminant analysis (FDA) of imaging data sets for identification of candidate markers of progressive disease in PCK rats. Our study highlights strong increases in lower mass lipids as main classifiers of cystic disease. Structure determination by high-resolution mass spectrometry identifies these altered lipids as taurine-conjugated bile acids. These sulfated lipids are selectively elevated in the PCK rat model but not in models of related hepatorenal fibrocystic diseases, suggesting that they be molecular markers of the disease and that a combination of MALDI imaging with high-resolution MS methods and Fisher discriminant data analysis may be applicable for lipid marker discovery.
Keywords:autosomal recessive polycystic kidney disease  imaging mass spectrometry  Fisher discriminant analysis  taurocholic acid  Fourier transform ion cyclotron resonance mass spectrometry  Matrix-assisted laser desorption/ionization
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