Amadori rearrangement products as potential biomarkers for inborn errors of amino-acid metabolism

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作者
Rianne E. van Outersterp
Sam J. Moons
Udo F. H. Engelke
Herman Bentlage
Tessa M. A. Peters
Arno van Rooij
Marleen C. D. G. Huigen
Siebolt de Boer
Ed van der Heeft
Leo A. J. Kluijtmans
Clara D. M. van Karnebeek
Ron A. Wevers
Giel Berden
Jos Oomens
Thomas J. Boltje
Karlien L. M. Coene
Jonathan Martens
机构
[1] Radboud University,Department of Laboratory Medicine, Translational Metabolic Laboratory
[2] Institute for Molecules and Materials,Department of Pediatrics, Radboud Center for Mitochondrial Medicine
[3] FELIX Laboratory,van’t Hoff Institute for Molecular Sciences
[4] Toernooiveld 7,undefined
[5] Radboud University,undefined
[6] Institute for Molecules and Materials,undefined
[7] Synthetic Organic Chemistry,undefined
[8] Radboud University Medical Center,undefined
[9] Radboud University Medical Center,undefined
[10] University of Amsterdam,undefined
来源
Communications Biology | / 4卷
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摘要
The identification of disease biomarkers plays a crucial role in developing diagnostic strategies for inborn errors of metabolism and understanding their pathophysiology. A primary metabolite that accumulates in the inborn error phenylketonuria is phenylalanine, however its levels do not always directly correlate with clinical outcomes. Here we combine infrared ion spectroscopy and NMR spectroscopy to identify the Phe-glucose Amadori rearrangement product as a biomarker for phenylketonuria. Additionally, we find analogous amino acid-glucose metabolites formed in the body fluids of patients accumulating methionine, lysine, proline and citrulline. Amadori rearrangement products are well-known intermediates in the formation of advanced glycation end-products and have been associated with the pathophysiology of diabetes mellitus and ageing, but are now shown to also form under conditions of aminoacidemia. They represent a general class of metabolites for inborn errors of amino acid metabolism that show potential as biomarkers and may provide further insight in disease pathophysiology.
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