Relationship Between Immunophenotypes, Genetic Profiles, and Clinicopathologic Characteristics in Small Bowel Adenocarcinoma.

Aitoshi Hoshimoto, Atsushi Tatsuguchi, Takeshi Yamada, Sho Kuriyama, Ryohei Hamakubo, Takayoshi Nishimoto, Jun Omori, Naohiko Akimoto, Katya Gudis, Keigo Mitsui, Shu Tanaka, Shunji Fujimori, Tsutomu Hatori, Akira Shimizu, Katsuhiko Iwakiri
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Abstract

Small bowel adenocarcinoma (SBA) is rare, and scant data exist regarding its molecular and clinicopathologic characteristics. This study aimed to clarify the correlation between immunophenotypes, DNA mismatch repair status, genomic profiling, and clinicopathologic characteristics in patients with SBA. We examined 68 surgical resections from patients with primary SBA for immunohistochemical analyses of CK7, CK20, CD10, CDX2, MUC1, MUC2, MUC4, MUC5AC, and MUC6 expression as well as mismatch repair status. Genomic profiling was performed on 30 cases using targeted next-generation sequencing. Tumor mucin phenotypes were classified as gastric, intestinal, gastrointestinal, or null based on MUC2, MUC5AC, MUC6, and CD10 immunostaining. The expression of these proteins was categorized into 3 classifications according to their relationship to: (1) tumor location: CK7/CK20, MUC4, and MUC6; (2) histologic type: mucinous adenocarcinoma was positive for MUC2 and negative for MUC6; and (3) TNM stage: CD10 was downregulated, whereas MUC1 was upregulated in advanced TNM stages. CDX2 was a specific marker for SBA generally expressed in the small intestine. MUC1 and MUC4 expression was significantly associated with worse prognosis. MUC2 expression correlated with better prognosis, except for mucinous adenocarcinoma. Although the difference was not statistically significant, gastric-type tumors were more frequently located in the duodenum and were absent in the ileum. APC and CTNNB1 mutations were not found in the gastric-type tumors. The SBA immunophenotype correlated with tumor location, biological behavior, and genomic alterations. Our results suggest that the molecular pathway involved in carcinogenesis of gastric-type SBA differs from that of intestinal-type SBA.
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小肠腺癌的免疫表型、遗传特征和临床病理特征之间的关系
小肠腺癌(SBA)非常罕见,有关其分子和临床病理特征的数据也很少。本研究旨在阐明小肠腺癌患者的免疫表型、DNA错配修复状态、基因组图谱和临床病理特征之间的相关性。我们检查了 68 例原发性 SBA 患者的手术切片,对 CK7、CK20、CD10、CDX2、MUC1、MUC2、MUC4、MUC5AC 和 MUC6 的表达以及错配修复状态进行了免疫组化分析。利用靶向新一代测序技术对30个病例进行了基因组分析。根据MUC2、MUC5AC、MUC6和CD10免疫染色,将肿瘤粘蛋白表型分为胃型、肠型、胃肠型和无效型。根据这些蛋白的表达与以下方面的关系,将其分为 3 类:(1) 肿瘤位置:CK7/CK20、MUC4 和 MUC6;(2) 组织学类型:粘液腺癌 MUC2 阳性,MUC6 阴性;(3) TNM 分期:CD10下调,而MUC1在TNM晚期上调。CDX2是SBA的特异性标志物,一般在小肠中表达。MUC1和MUC4的表达与较差的预后显著相关。除粘液腺癌外,MUC2的表达与较好的预后相关。虽然差异没有统计学意义,但胃型肿瘤更多地位于十二指肠,而回肠则没有。胃型肿瘤中未发现 APC 和 CTNNB1 突变。SBA 免疫表型与肿瘤位置、生物学行为和基因组改变相关。我们的研究结果表明,胃型 SBA 与肠型 SBA 发生癌变的分子途径不同。
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