Molecular characterization of Barrett’s esophagus at single-cell resolution

Author:

Busslinger Georg A.ORCID,de Barbanson Buys,Oka RurikaORCID,Weusten Bas L. A.,de Maat Michiel,van Hillegersberg Richard,Brosens Lodewijk A. A.,van Boxtel RubenORCID,van Oudenaarden Alexander,Clevers HansORCID

Abstract

Barrett’s esophagus (BE) is categorized, based on morphological appearance, into different stages, which correlate with the risk of developing esophageal adenocarcinoma. More advanced stages are more likely to acquire chromosomal instabilities, but stage-specific markers remain elusive. Here, we performed single-cell DNA-sequencing experiments (scDNAseq) with fresh BE biopsies. Dysplastic BE cells frequently contained chromosomal instability (CIN) regions, and these CIN cells carried mutations corresponding to the COSMIC mutational signature SBS17, which were not present in biopsy-matched chromosomally stable (CS) cells or patient-matched nondiseased control cells. CS cells were predominantly found in nondysplastic BE biopsies. The single-base substitution (SBS) signatures of all CS BE cells analyzed were indistinguishable from those of nondiseased esophageal or gastric cells. Single-cell RNA-sequencing (scRNAseq) experiments with BE biopsies identified two sets of marker genes which facilitate the distinction between columnar BE epithelium and nondysplastic/dysplastic stages. Moreover, histological validation confirmed a correlation between increased CLDN2 expression and the presence of dysplastic BE stages. Our scDNAseq and scRNAseq datasets, which are a useful resource for the community, provide insight into the mutational landscape and gene expression pattern at different stages of BE development.

Funder

Advanced Grant ERC-AdG

NWO-ZonMw

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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