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Stable isotope-assisted untargeted metabolomics identifies ALDH1A1-driven erythronate accumulation in lung cancer cells

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Item Type:Article
Title:Stable isotope-assisted untargeted metabolomics identifies ALDH1A1-driven erythronate accumulation in lung cancer cells
Creators Name:Zhang, J. and Keibler, M.A. and Dong, W. and Ghelfi, J. and Cordes, T. and Kanashova, T. and Pailot, A. and Linster, C.L. and Dittmar, G. and Metallo, C.M. and Lautenschlaeger, T. and Hiller, K. and Stephanopoulos, G.
Abstract:Using an untargeted stable isotope-assisted metabolomics approach, we identify erythronate as a metabolite that accumulates in several human cancer cell lines. Erythronate has been reported to be a detoxification product derived from off-target glycolytic metabolism. We use chemical inhibitors and genetic silencing to define the pentose phosphate pathway intermediate erythrose 4-phosphate (E4P) as the starting substrate for erythronate production. However, following enzyme assay-coupled protein fractionation and subsequent proteomics analysis, we identify aldehyde dehydrogenase 1A1 (ALDH1A1) as the predominant contributor to erythrose oxidation to erythronate in cell extracts. Through modulating ALDH1A1 expression in cancer cell lines, we provide additional support. We hence describe a possible alternative route to erythronate production involving the dephosphorylation of E4P to form erythrose, followed by its oxidation by ALDH1A1. Finally, we measure increased erythronate concentrations in tumors relative to adjacent normal tissues from lung cancer patients. These findings suggest the accumulation of erythronate to be an example of metabolic reprogramming in cancer cells, raising the possibility that elevated levels of erythronate may serve as a biomarker of certain types of cancer.
Keywords:Cancer Metabolism, Untargeted Metabolomics, Erythronate, Pentose Phosphate Pathway, Aldehyde Dehydrogenase 1A1 (ALDH1A1)
Source:Biomedicines
ISSN:2227-9059
Publisher:MDPI
Volume:11
Number:10
Page Range:2842
Date:19 October 2023
Official Publication:https://doi.org/10.3390/biomedicines11102842
PubMed:View item in PubMed

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