Goblet Cell Ratio in Combination with Differentiation and Stem Cell Markers in Barrett Esophagus Allow Distinction of Patients with and without Esophageal Adenocarcinoma

Schellnegger, Raphael; Quante, Anne S.; Rospleszcz, Susanne; Schernhammer, Martina; Höhl, Bettina; Tobiasch, Moritz; Pastula, Agniezska; Brandtner, Anna; Abrams, Julian A.; Strauch, Konstantin; Schmid, Roland M.; Wang, Yichen; Quante, Michael

doi:10.1158/1940-6207.capr-16-0117

Cited by 19 publications

(18 citation statements)

References 45 publications

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“…However, this result unequivocally shows that intestinal metaplasia is not the sole precursor to cancer in the metaplastic distal oesophagus. In fact, recent studies have suggested that progression to cancer may occur less often in patients with higher goblet cell counts [ 32 , 33 ]. This suggests that goblet cell differentiation may in fact protect against neoplastic transformation.…”

Section: What Is the Origin Of Barrett’s Cancer?mentioning

confidence: 99%

The metaplastic mosaic of Barrett’s oesophagus

et al. 2018

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Barrett’s oesophagus surveillance biopsies represent a significant share of the daily workload for a busy histopathology department. Given the emphasis on endoscopic detection and dysplasia grading, it is easy to forget that the benefits of these screening programs remain unproven. The majority of patients are at low risk of progression to oesophageal adenocarcinoma, and periodic surveillance of these patients is burdensome and costly. Here, we investigate the parallels in the development of Barrett’s oesophagus and other scenarios of wound healing in the intestine. There is now increased recognition of the full range of glandular phenotypes that can be found in patients’ surveillance biopsies, and emerging evidence suggests parallel pathways to oesophageal adenocarcinoma. Greater understanding of the conditions that favour progression to cancer in the distal oesophagus will allow us to focus resources on patients at increased risk.

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Section: What Is the Origin Of Barrett’s Cancer?mentioning

confidence: 99%

The metaplastic mosaic of Barrett’s oesophagus

et al. 2018

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“…In this mouse model, exposure of the esophagus to bile acids accelerates the development of Barrett-like metaplasia and dysplasia, through a mechanism involving a strong activation of the NOTCH signaling pathway [ 91 ]. The analysis of this mouse model allowed also to explore the cell progenitor involved in the development of Barrett metaplasia, providing evidence in favor of a possible involvement of gastric cardia progenitor cells [ 92 ]. The analysis of this mouse model of Barrett’s esophagus provided evidence that increasing stem cell marker LGR5 and niche cell marker DCLK1 and decreasing differentiation marker (secretory mucus cells, TFF2 + cells) correlated with a high tumor score [ 92 ].…”

Section: Cellular Origin Of Barrett’s Esophagusmentioning

confidence: 99%

“…The analysis of this mouse model allowed also to explore the cell progenitor involved in the development of Barrett metaplasia, providing evidence in favor of a possible involvement of gastric cardia progenitor cells [ 92 ]. The analysis of this mouse model of Barrett’s esophagus provided evidence that increasing stem cell marker LGR5 and niche cell marker DCLK1 and decreasing differentiation marker (secretory mucus cells, TFF2 + cells) correlated with a high tumor score [ 92 ]. In a subsequent study, it was tested the applicability of these markers for human Barrett’s esophagus, particularly for distinguishing patients with Barrett’s esophagus with no evidence of dysplasia from those with dysplasia [ 92 ].…”

Section: Cellular Origin Of Barrett’s Esophagusmentioning

confidence: 99%

“…The analysis of this mouse model of Barrett’s esophagus provided evidence that increasing stem cell marker LGR5 and niche cell marker DCLK1 and decreasing differentiation marker (secretory mucus cells, TFF2 + cells) correlated with a high tumor score [ 92 ]. In a subsequent study, it was tested the applicability of these markers for human Barrett’s esophagus, particularly for distinguishing patients with Barrett’s esophagus with no evidence of dysplasia from those with dysplasia [ 92 ]. Low levels of TFF2 supported the best discrimination between nondysplastic Barrett’s esophagus and Barrett’s esophagus with cancer, followed by high levels of DCLK1, low goblet ratio and high LGR5 expression [ 92 ].…”

Section: Cellular Origin Of Barrett’s Esophagusmentioning

confidence: 99%

“…In a subsequent study, it was tested the applicability of these markers for human Barrett’s esophagus, particularly for distinguishing patients with Barrett’s esophagus with no evidence of dysplasia from those with dysplasia [ 92 ]. Low levels of TFF2 supported the best discrimination between nondysplastic Barrett’s esophagus and Barrett’s esophagus with cancer, followed by high levels of DCLK1, low goblet ratio and high LGR5 expression [ 92 ]. These findings support a risk prediction model of cancer progression of Barrett’s esophagus.…”

Section: Cellular Origin Of Barrett’s Esophagusmentioning

confidence: 99%

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Esophageal Cancer: Genomic and Molecular Characterization, Stem Cell Compartment and Clonal Evolution

2017

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Esophageal cancer (EC) is the eighth most common cancer and is the sixth leading cause of death worldwide. The incidence of histologic subtypes of EC, esophageal adenocarcinoma (EAC) and esophageal squamous carcinoma (ESCC), display considerable geographic variation. EAC arises from metaplastic Barrett’s esophagus (BE) in the context of chronic inflammation secondary to exposure to acid and bile. The main risk factors for developing ESCC are cigarette smoking and alcohol consumption. The main somatic genetic abnormalities showed a different genetic landscape in EAC compared to ESCC. EAC is a heterogeneous cancer dominated by copy number alterations, a high mutational burden, co-amplification of receptor tyrosine kinase, frequent TP53 mutations. The cellular origins of BE and EAC are still not understood: animal models supported a cellular origin either from stem cells located in the basal layer of esophageal epithelium or from progenitors present in the cardia region. Many studies support the existence of cancer stem cells (CSCs) able to initiate and maintain EAC or ESCC. The exact identification of these CSCs, as well as their role in the pathogenesis of EAC and ESCC remain still to be demonstrated. The reviewed studies suggest that current molecular and cellular characterization of EAC and ESCC should serve as background for development of new treatment strategies.

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Barrett's esophagus: The pathomorphological and molecular genetic keystones of neoplastic progression

et al. 2021

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Barrett's esophagus is a widespread chronically progressing disease of heterogeneous nature. A life threatening complication of this condition is neoplastic transformation, which is often overlooked due to lack of standardized approaches in diagnosis, preventative measures and treatment. In this essay, we aim to stratify existing data to show specific associations between neoplastic transformation and the underlying processes which predate cancerous transition. We discuss pathomorphological, genetic, epigenetic, molecular and immunohistochemical methods related to neoplasia detection on the basis of Barrett's esophagus. Our review sheds light on pathways of such neoplastic progression in the distal esophagus, providing valuable insight into progression assessment, preventative targets and treatment modalities. Our results suggest that molecular, genetic and epigenetic alterations in the esophagus arise earlier than cancerous transformation, meaning the discussed targets can help form preventative strategies in at-risk patient groups.

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Goblet Cell Ratio in Combination with Differentiation and Stem Cell Markers in Barrett Esophagus Allow Distinction of Patients with and without Esophageal Adenocarcinoma

Cited by 19 publications

References 45 publications

The metaplastic mosaic of Barrett’s oesophagus

The metaplastic mosaic of Barrett’s oesophagus

Esophageal Cancer: Genomic and Molecular Characterization, Stem Cell Compartment and Clonal Evolution

Barrett's esophagus: The pathomorphological and molecular genetic keystones of neoplastic progression

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