Suprabasal cells retain progenitor cell identity programs in eosinophilic esophagitis–driven basal cell hyperplasia
Margarette H. Clevenger, … , Kelly A. Whelan, Marie-Pier Tétreault
Margarette H. Clevenger, … , Kelly A. Whelan, Marie-Pier Tétreault
Published September 6, 2023
Citation Information: JCI Insight. 2023;8(19):e171765. https://doi.org/10.1172/jci.insight.171765.
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Research Article Gastroenterology Inflammation

Suprabasal cells retain progenitor cell identity programs in eosinophilic esophagitis–driven basal cell hyperplasia

Abstract

Eosinophilic esophagitis (EoE) is an esophageal immune-mediated disease characterized by eosinophilic inflammation and epithelial remodeling, including basal cell hyperplasia (BCH). Although BCH is known to correlate with disease severity and with persistent symptoms in patients in histological remission, the molecular processes driving BCH remain poorly defined. Here, we demonstrate that BCH is predominantly characterized by an expansion of nonproliferative suprabasal cells that are still committed to early differentiation. Furthermore, we discovered that suprabasal and superficial esophageal epithelial cells retain progenitor identity programs in EoE, evidenced by increased quiescent cell identity scoring and the enrichment of signaling pathways regulating stem cell pluripotency. Enrichment and trajectory analyses identified SOX2 and KLF5 as potential drivers of the increased quiescent identity and epithelial remodeling observed in EoE. Notably, these alterations were not observed in gastroesophageal reflux disease. These findings provide additional insights into the differentiation process in EoE and highlight the distinct characteristics of suprabasal and superficial esophageal epithelial cells in the disease.

Authors

Margarette H. Clevenger, Adam L. Karami, Dustin A. Carlson, Peter J. Kahrilas, Nirmala Gonsalves, John E. Pandolfino, Deborah R. Winter, Kelly A. Whelan, Marie-Pier Tétreault

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Figure 8

Pseudotemporal trajectory-dependent gene programs are altered in EEC in EoE.

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Pseudotemporal trajectory-dependent gene programs are altered in EEC in ...
(A) Average signature score Z scores per EoE trajectory–dependent module for each epithelial cluster in HC or EoE. Color intensity indicates relative scoring. (B) UMAP of the merged scRNA-Seq data set of EEC from HC or EoE, colored by module 7 gene signature score. (C) Enriched pathways for module 7 genes, ranked by P value. Color intensity indicates the percentage of module 7 genes along each pathway. (D) Expression of SOX2, KLF5, or module 7 genes across EEC and percentage of EEC expressing meaningful levels of all 3 conditions, ordered by pseudotime for both HC and EoE. Lines represent moving averages calculated by LOESS regression. B, Basal; Q, Quiescent; BD, Basal_Dividing; EB, Epibasal; SB, Suprabasal; SF, Superficial.