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Aldehyde-mediated inhibition of asparagine biosynthesis has implications for diabetes and alcoholism

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posted on 2024-02-06, 10:29 authored by Tobias John, Nadia Saffoon, John Walsby-Tickle, Svenja S Hester, Felix A Dingler, Christopher L Millington, James SO McCullagh, Ketan J Patel, Richard J Hopkinson, Christopher J Schofield

Patients with alcoholism and type 2 diabetes manifest altered metabolism, including elevated aldehyde levels and unusually low asparagine levels. We show that asparagine synthetase B (ASNS), the only human asparagine-forming enzyme, is inhibited by disease-relevant reactive aldehydes, including formaldehyde and acetaldehyde. Cellular studies show non-cytotoxic amounts of reactive aldehydes induce a decrease in asparagine levels. Biochemical analyses reveal inhibition results from reaction of the aldehydes with the catalytically important N-terminal cysteine of ASNS. The combined cellular and biochemical results suggest a possible mechanism underlying the low asparagine levels in alcoholism and diabetes. The results will stimulate research on the biological consequences of the reactions of aldehydes with nucleophilic residues.

Funding

Industrial CASE Account - University of Oxford 2017

Engineering and Physical Sciences Research Council

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Oxford Genomics Centre at the Wellcome Centre for Human Genetics (funded by Wellcome Trust grant ref. 203141/Z/16/Z)

Cancer Research UK (C8717/A18245)

Profiling the effect of the metabolite formaldehyde during gemcitabine chemotherapy

Wellcome Trust

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Defining the physiology and therapeutic potential of oxygenases as signalling enzymes.

Wellcome Trust

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History

Author affiliation

School of Chemistry, University of Leicester

Version

  • VoR (Version of Record)

Published in

Chemical Science

Publisher

Royal Society of Chemistry (RSC)

issn

2041-6520

eissn

2041-6539

Copyright date

2024

Available date

2024-02-06

Language

en

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    University of Leicester Publications

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