Variability in morphology and immunohistochemistry of Crohn's disease-associated small bowel neoplasms: implications of Claudin 18 and Cadherin 17 expression for tumor-targeted immunotherapies.

IF 3.4 3区医学 Q1 PATHOLOGY

Virchows Archiv Pub Date : 2024-08-21 DOI:10.1007/s00428-024-03896-4

Mai Iwaya, Makoto Kodama, Keiko Abe, Kahoko Maeda, Tomoyuki Nakajima, Takeshi Uehara, Risa Nishio, Tetsuo Yamana, Robert Riddell, Hiroyoshi Ota

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Abstract

Aims: Inflammatory bowel disease-associated colorectal carcinomas are known to have different morphology, immunoprofile, and genetic findings from sporadic colorectal carcinomas; however, little is known for Crohn's disease-associated small bowel neoplasms (CD-SBNs). Cadherin 17 is a useful biomarker of adenocarcinomas with intestinal phenotype and recently reported as an ideal target for chimeric antigen receptor T-cells (CAR-T) therapy for gastrointestinal carcinoma. Claudin 18 is a cell adhesion protein, and Claudin18 isoform 2 (CLDN18.2) is frequently expressed at high levels in gastric-type adenocarcinoma. Zolbetuximab, a targeted monoclonal antibody, has been developed for CLDN18.2-positive gastroesophageal adenocarcinoma. We examined a series of CD-SBNs for both Cadherin 17 and Claudin 18, and also hypothesized that expression of Claudin 18 was associated with gastric phenotype.

Methods and results: We performed histological and immunohistochemical examinations on 25 CD-SBNs. Most of adenocarcinomas showed tubular morphology as seen in gastric carcinomas, whereas a subset of dysplasia was morphologically similar to that of the large bowel. Cadherin17 and Claudin 18 expression was identified in 93% and 57% CD-associated adenocarcinomas respectively. In Cadherin 17-positive CD-SBNs, frequent MUC5AC, MUC6, and Claudin18 expression was identified (61%, 57%, and 57%, respectively). Claudin 18-positive CD-SBNs showed significantly more MUC5AC and MUC6 expression than Claudin 18-negative CD-SBNs (P = 0.005, < 0.001 respectively).

Conclusion: In CD-associated small bowel adenocarcinomas, Cadherin 17 expression was frequently retained and Claudin 18 was frequently co-expressed. Claudin 18 had a positive correlation with the expression of gastric mucins. These results suggest that CD-associated small bowel adenocarcinomas may be candidates for Cadherin 17- and Claudin 18-targeted immunotherapies.

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克罗恩病相关小肠肿瘤的形态和免疫组化差异：Claudin 18 和 Cadherin 17 的表达对肿瘤靶向免疫疗法的影响。

目的：众所周知，与炎症性肠病相关的结直肠癌在形态、免疫谱和遗传学结果上与散发性结直肠癌不同；然而，人们对与克罗恩病相关的小肠肿瘤（CD-SBN）却知之甚少。粘连蛋白 17 是具有肠表型的腺癌的有用生物标志物，最近有报道称它是嵌合抗原受体 T 细胞（CAR-T）治疗胃肠癌的理想靶点。Claudin 18是一种细胞粘附蛋白，Claudin18异构体2（CLDN18.2）经常在胃型腺癌中高水平表达。针对CLDN18.2阳性的胃食管腺癌开发了靶向单克隆抗体唑贝妥昔单抗。我们对一系列 CD-SBN 进行了检查，检测了 Cadherin 17 和 Claudin 18，并假设 Claudin 18 的表达与胃表型有关：我们对 25 例 CD-SBN 进行了组织学和免疫组化检查。结果：我们对 25 例 CD-SBN 进行了组织学和免疫组化检查，大部分腺癌表现出与胃癌相同的管状形态，而一部分发育不良的腺癌在形态上与大肠癌相似。93%和57%的CD相关腺癌中分别发现了Cadherin17和Claudin18的表达。在Cadherin 17阳性的CD-SBNs中，MUC5AC、MUC6和Claudin18表达频繁（分别为61%、57%和57%）。Claudin 18 阳性的 CD-SBNs 的 MUC5AC 和 MUC6 表达明显多于 Claudin 18 阴性的 CD-SBNs（P = 0.005，结论：在 CD 相关小肠腺癌中，Cadherin 17 的表达经常被保留，而 Claudin 18 则经常同时表达。Claudin 18与胃粘蛋白的表达呈正相关。这些结果表明，CD相关小肠腺癌可能是Cadherin 17和Claudin 18靶向免疫疗法的候选者。

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来源期刊

Virchows Archiv 医学-病理学

CiteScore

7.40

自引率

2.90%

发文量

204

审稿时长

4-8 weeks

期刊介绍： Manuscripts of original studies reinforcing the evidence base of modern diagnostic pathology, using immunocytochemical, molecular and ultrastructural techniques, will be welcomed. In addition, papers on critical evaluation of diagnostic criteria but also broadsheets and guidelines with a solid evidence base will be considered. Consideration will also be given to reports of work in other fields relevant to the understanding of human pathology as well as manuscripts on the application of new methods and techniques in pathology. Submission of purely experimental articles is discouraged but manuscripts on experimental work applicable to diagnostic pathology are welcomed. Biomarker studies are welcomed but need to abide by strict rules (e.g. REMARK) of adequate sample size and relevant marker choice. Single marker studies on limited patient series without validated application will as a rule not be considered. Case reports will only be considered when they provide substantial new information with an impact on understanding disease or diagnostic practice.