Claudin-18 expression in small bowel adenocarcinoma: a clinico-pathologic study

被引:0
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作者
Giovanni Arpa
Matteo Fassan
Camilla Guerini
Erica Quaquarini
Federica Grillo
Valentina Angerilli
Vincenza Guzzardo
Sara Lonardi
Francesca Bergamo
Marco Vincenzo Lenti
Paolo Pedrazzoli
Marco Paulli
Antonio Di Sabatino
Alessandro Vanoli
机构
[1] University of Pavia,Department of Molecular Medicine, Unit of Anatomic Pathology
[2] Anatomic Pathology Unit,Department of Medicine
[3] Fondazione IRCCS San Matteo Hospital,Medical Oncology Unit
[4] DIMED,Pathology Unit, Department of Surgical and Diagnostic Sciences (DISC)
[5] University of Padua,Department of Oncology
[6] Veneto Institute of Oncology,First Department of Internal Medicine
[7] IOV-IRCCS,undefined
[8] ICS Maugeri-IRCCS SpA SB,undefined
[9] University of Genoa,undefined
[10] IRCCS Ospedale Policlinico San Martino,undefined
[11] Veneto Institute of Oncology,undefined
[12] IOV-IRCCS,undefined
[13] San Matteo Hospital Foundation,undefined
[14] University of Pavia,undefined
[15] Oncology Unit,undefined
[16] IRCCS San Matteo Hospital,undefined
来源
Virchows Archiv | 2022年 / 481卷
关键词
Coeliac disease; Crohn’s disease; Gastric markers; Immune-mediated disorder; Small intestine;
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学科分类号
摘要
Non-ampullary small bowel adenocarcinoma is a rare neoplasm with an ominous prognosis, whose incidence is higher in some chronic immuno-inflammatory conditions, such as coeliac and Crohn’s disease. Recently, claudin 18.2, a transmembrane protein normally expressed in gastric mucosa, has been recognized as a novel pan-cancer therapeutic target, and several clinical trials with claudin-18-directed drugs have shown promising results on various gastrointestinal malignancies. This is the first study focusing on claudin-18 expression in small bowel adenocarcinomas. The immunohistochemical expression of claudin-18 (clone 43-14A) was assessed in 81 small bowel adenocarcinomas of diverse aetiologies and correlated with several clinico-pathologic features and patient survival. We found that 28% of adenocarcinomas were immunoreactive for claudin-18, with cutoff values of ≥1% at any intensity, while 6% of cancers showed immunoexpression of ≥75% with 2+/3+ score. Moreover, claudin-18 (≥1%) was positively associated with cytokeratin 7 (CK7) and MUC5AC expression, showing CK7+/MUC5AC+ carcinomas the highest rate of positive cases, whereas a negative correlation was found between claudin-18 and CDX2 expression. In addition, some cancer-adjacent dysplastic growths and foci of gastric-type metaplasia in Crohn’s disease-associated cases showed claudin-18 immunoreactivity. Survival analysis showed a non-significant trend towards a worse cancer-specific survival for claudin-18-positive cases. A fraction of small bowel adenocarcinomas, mainly sporadic or Crohn’s disease-associated, and often exhibiting a non-intestinal immunoprofile, expressed claudin-18, suggesting that claudin-18-directed targeted therapy is worth investigating in such cancers.
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页码:853 / 863
页数:10
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