Eosinophilic esophagitis-associated epithelial remodeling may limit esophageal carcinogenesis

Annie D Fuller; Adam L Karami; Mohammad Faujul Kabir; Alena Klochkova; Jazmyne L Jackson; Anbin Mu; Yinfei Tan; Andres J Klein-Szanto; Kelly A Whelan

doi:10.3389/falgy.2023.1086032

Eosinophilic esophagitis-associated epithelial remodeling may limit esophageal carcinogenesis

Front Allergy. 2023 Mar 29:4:1086032. doi: 10.3389/falgy.2023.1086032. eCollection 2023.

Authors

Annie D Fuller¹, Adam L Karami¹, Mohammad Faujul Kabir¹, Alena Klochkova¹, Jazmyne L Jackson¹, Anbin Mu¹, Yinfei Tan², Andres J Klein-Szanto³, Kelly A Whelan^{1

4}

Affiliations

¹ Fels Cancer Institute for Personalized Medicine, Temple University Lewis Katz School of Medicine, Philadelphia, PA, United States.
² Genomics Facility, Fox Chase Cancer Center, Philadelphia, PA, United States.
³ Histopathology Facility, Fox Chase Cancer Center, Philadelphia, PA, United States.
⁴ Department of Cancer & Cellular Biology, Temple University Lewis Katz School of Medicine, Philadelphia, PA, United States.

Abstract

Introduction: Under homeostatic conditions, esophageal epithelium displays a proliferation/differentiation gradient that is generated as proliferative basal cells give rise to suprabasal cells then terminally differentiated superficial cells. This proliferation/differentiation gradient is often perturbed in esophageal pathologies. Basal cell hyperplasia may occur in patients with gastroesophageal reflux disease (GERD), a condition in which acid from the stomach enters the esophagus, or eosinophilic esophagitis (EoE), an emerging form of food allergy. While GERD is a primary risk factor for esophageal cancer, epidemiological data suggests that EoE patients do not develop esophageal cancer.

Methods: In order to investigate the impact of EoE and esophageal cancer specifically on the cellular landscape of esophageal epithelium, we perform single cell RNA-sequencing in murine models of EoE and esophageal cancer, specifically esophageal squamous cell carcinoma (ESCC). We further evaluate modules of co-expressed genes in EoE- and ESCC-enriched epithelial cell clusters. Finally, we pair EoE and ESCC murine models to examine the functional relationship between these pathologies.

Results: In mice with either EoE or ESCC, we find expansion of cell populations as compared to normal esophageal epithelium. In mice with EoE, we detect distinct expansion of 4 suprabasal populations coupled with depletion of 2 basal populations. By contrast, mice with ESCC display unique expansion of 2 basal populations and 1 suprabasal population, as well as depletion of 2 suprabasal populations. Senescence, glucocorticoid receptor signaling, and granulocyte-macrophage colony-stimulating factor pathways are associated with EoE-enriched clusters while pathways associated with cell proliferation and metabolism are identified in ESCC-enriched clusters. Finally, our in vivo data demonstrate that exposure to EoE inflammation limits tumor burden of esophageal carcinogenesis.

Discussion: Our findings provide the first functional investigation of the relationship between EoE and esophageal cancer and suggest that esophageal epithelial remodeling events occurring in response to EoE inflammation may limit esophageal carcinogenesis. This investigation may have future implications for leveraging allergic inflammation-associated alterations in epithelial biology to prevent and/or treat esophageal cancer.

Keywords: atopy; cell differentiation; cell fate trajectory; eosinophilic esophagitis; esophageal epithelium; esophageal squamous cell carcinoma.

Abstract

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