Endogenous aldehyde accumulation generates genotoxicity and exhaled biomarkers in esophageal adenocarcinoma

Author:

Antonowicz StefanORCID,Bodai Zsolt,Wiggins Tom,Markar Sheraz R.,Boshier Piers R.,Goh Yan MeiORCID,Adam Mina E.,Lu Haonan,Kudo Hiromi,Rosini Francesca,Goldin RobertORCID,Moralli DanielaORCID,Green Catherine M.,Peters Chris J.,Habib Nagy,Gabra HaniORCID,Fitzgerald Rebecca C.ORCID,Takats Zoltan,Hanna George B.ORCID

Abstract

AbstractVolatile aldehydes are enriched in esophageal adenocarcinoma (EAC) patients’ breath and could improve early diagnosis, however the mechanisms of their production are unknown. Here, we show that weak aldehyde detoxification characterizes EAC, which is sufficient to cause endogenous aldehyde accumulation in vitro. Two aldehyde groups are significantly enriched in EAC biopsies and adjacent tissue: (i) short-chain alkanals, and (ii) medium-chain alkanals, including decanal. The short-chain alkanals form DNA-adducts, which demonstrates genotoxicity and confirms inadequate detoxification. Metformin, a putative aldehyde scavenger, reduces this toxicity. Tissue and breath concentrations of the medium-chain alkanal decanal are correlated, and increased decanal is linked to reduced ALDH3A2 expression, TP53 deletion, and adverse clinical features. Thus, we present a model for increased exhaled aldehydes based on endogenous accumulation from reduced detoxification, which also causes therapeutically actionable genotoxicity. These results support EAC early diagnosis trials using exhaled aldehyde analysis.

Funder

DH | National Institute for Health Research

Rosetrees Trust

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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