Claudin-18

Mary T Wong; Aatur D Singhi; Brent K Larson; Carissa A T Huynh; Bonnie L Balzer; Miguel Burch; Deepti Dhall; Alexandra Gangi; Jun Gong; Maha Guindi; Andrew E Hendifar; Stacey A Kim; Mariza de Peralta-Venturina; Kevin M Waters

doi:10.5858/arpa.2021-0428-OA

Claudin-18

Arch Pathol Lab Med. 2022 May 1;147(5):559-567. doi: 10.5858/arpa.2021-0428-OA.

Authors

Affiliations

¹ From the Department of Pathology, Oregon Health & Science University, Portland (Wong).
² From the Department of Pathology, School of Medicine, University of Pittsburgh, Pittsburgh, Pennsylvania (Singhi).
³ From the Department of Pathology and Laboratory Medicine (Larson, Huynh, Balzer, Guindi, Kim, de Peralta-Venturina, Waters).
⁴ From the Division of Surgical Oncology, Department of Surgery (Burch, Gangi), Samuel Oschin Comprehensive Cancer Institute.
⁵ From Cedars-Sinai Medical Center, Los Angeles, California; and the Department of Pathology, University of Alabama at Birmingham (Dhall).
⁶ From the Department of Medicine, Division of Hematology and Oncology (Gong, Hendifar), Samuel Oschin Comprehensive Cancer Institute.

PMID: 35976638
DOI: 10.5858/arpa.2021-0428-OA

Abstract

Context.—: Claudin-18 is expressed in some gastric cancers. Clinical trials are evaluating it as a therapeutic target.

Objectives.—: To evaluate claudin-18 expression in intestinal metaplasia, dysplasia, and adenocarcinoma of the distal esophagus/gastroesophageal junction and stomach and to evaluate claudin-18 expression in gastric and nongastric neuroendocrine tumors as a marker of gastric origin.

Design.—: Samples included gastroesophageal junction with intestinal metaplasia (n = 40), dysplasia (n = 54), and adenocarcinoma (n = 20) and stomach with intestinal metaplasia (n = 79), dysplasia (n = 43), and adenocarcinoma (n = 25). Additionally, gastric (n = 40) and nongastric (n = 322) neuroendocrine tumors were included. Claudin-18 expression was evaluated for any staining as positive and by meeting clinical trial inclusion criteria (≥2+ intensity in ≥50% of tumor).

Results.—: Claudin-18 staining was not significantly different across dysplasia categories in the gastroesophageal junction (P = .11) or stomach (P = .12). The rate of positive staining was higher in gastroesophageal junction than stomach for intestinal metaplasia (37 of 40 [92.5%] versus 37 of 79 [46.8%]; P < .001) and high-grade dysplasia (33 of 38 [86.8%] versus 9 of 16 [56.3%]; P = .03). Intestinal metaplasia showed staining in 7 of 37 autoimmune gastritis samples (18.9%) compared with 30 of 42 samples without autoimmune gastritis (71.4%) (P < .001). Adenocarcinoma showed similar staining in gastroesophageal junction (15 of 20; 75.0%) and stomach (17 of 25; 68.0%) (P = .85). Eighty percent (32 of 40) of gastric neuroendocrine tumors were positive for claudin-18 expression, with 57.5% (23 of 40) meeting clinical trial inclusion criteria. Comparatively, 0.62% (2 of 322) of nongastric neuroendocrine tumors showed staining (P < .001).

Conclusions.—: Claudin-18 staining was similar in intestinal metaplasia, dysplasia, and adenocarcinoma. Claudin-18 was negative in most cases of intestinal metaplasia in autoimmune gastritis, indicating that intestinal metaplasia in this setting may differ from other forms. Claudin-18 was sensitive and specific for gastric origin in neuroendocrine tumors.

MeSH terms

Adenocarcinoma* / pathology
Claudins
Esophagogastric Junction / pathology
Gastritis* / pathology
Humans
Hyperplasia / pathology
Metaplasia / pathology
Neuroendocrine Tumors* / pathology
Precancerous Conditions* / pathology
Stomach Neoplasms* / pathology

Substances

Claudins