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Stomach and Intestine(Tokyo) Volume 50, Issue 12 （November 2015）

胃と腸 50巻12号（2015年11月発行）

Japanese English

今月の主題胃底腺型胃癌

主題研究

胃底腺型胃癌の発育進展様式と発癌機序 Histological Characteristics of Neoplastic Progression and Molecular Changes in Gastric Adenocarcinoma of Fundic Gland Type 村上敬 ^1,2 , 三富弘之 ³ , 八尾隆史 ² , 野村亮介 ¹ , 李世容 ¹ , 上山浩也 ¹ , 日高康博 ¹ , 松本健史 ¹ , 齋藤剛 ² , 長田太郎 ¹ , 永原章仁 ⁴ , 渡辺純夫 ¹ Takashi Murakami ^1,2 , Hiroyuki Mitomi ³ , Takashi Yao ² , Ryosuke Nomura ¹ , Se-Yong Lee ¹ , Hiroya Ueyama ¹ , Yasuhiro Hidaka ¹ , Kenshi Matsumoto ¹ , Tsuyoshi Saito ² , Taro Osada ¹ , Akihito Nagahara ⁴ , Sumio Watanabe ¹ ¹順天堂大学医学部消化器内科 ²順天堂大学大学院医学研究科人体病理病態学 ³関東労災病院病理診断科 ⁴順天堂大学医学部附属静岡病院消化器内科 ¹Department of Gastroenterology, Juntendo University School of Medicine, Tokyo ²Department of Human Pathology, Juntendo University School of Medicine, Tokyo ³Department of Pathology, Kanto Rosai Hospital, Kawasaki, Japan ⁴Department of Gastroenterology, Juntendo University Shizuoka Hospital, Izunokuni, Japan キーワード：胃底腺型胃癌 , Wnt/β-cateninシグナル , GNAS , Kras , GTP結合蛋白 Keyword: 胃底腺型胃癌 , Wnt/β-cateninシグナル , GNAS , Kras , GTP結合蛋白 pp.1559-1565

発行日 2015年11月25日 Published Date 2015/11/25

DOI https://doi.org/10.11477/mf.1403200472

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要旨●胃底腺型胃癌のβ-catenin核内標識率は浸潤に伴い増加し，胃底腺ポリープ，通常型胃癌より高く，Wnt/β-cateninシグナル伝達系関連遺伝子の変異はAXIN2（27％），CTNNB1（15％），PPP2R1A（9％）と胃底腺ポリープや通常型胃癌より高率で，さらに同伝達系関連のSFRP1，APC，AXIN2遺伝子のメチル化率（67〜89％）も胃底腺ポリープより高い．また，胃底腺型胃癌（粘膜下層浸潤癌）ではGNAS遺伝子変異（19％），Kras遺伝子変異（8％）を認めるが，胃底腺ポリープや通常型胃癌ではほとんどみられない．以上から，胃底腺型胃癌の発育進展には胃底腺ポリープや通常型胃癌とは異なるWnt系およびGTP結合蛋白関連シグナル伝達系の活性化が関与すると考えられる．

　GA-FG（gastric adenocarcinoma of fundic gland type）is a newly described, rare variant of gastric carcinoma with less aggressive biological behavior, and it is predominantly composed of chief cells with anisonucleosis. Nuclear β-catenin immunolabeling in GA-FG showed a stepwise increment from intramucosal tumors to submucosal invasive carcinoma, and was higher than those seen in fundic gland polyps or conventional gastric carcinomas. Analysis of members of the Wnt/β-catenin signaling pathway indicated that AXIN2, CTNNB1（the gene that encodes for β-catenin）, or PPP2R1A（protein phosphatase 2 regulatory protein 1A, the gene that encodes for protein phosphatase 2）were mutated in 27%, 15%, and 9% of GA-FG cases, respectively ; these frequencies were higher than those seen in fundic gland polyps or conventional gastric carcinomas. SFRP1（another gene member of the Wnt/β-catenin signal pathway）, APC, and AXIN2 were methylated in 67-89% of GA-FGs, which was higher than that seen in fundic gland polyps. Activating mutations in GNAS and Kras were detected in 19% and 8% of GA-FGs, respectively, whereas these mutations were found very rarely in fundic gland polyps or conventional gastric carcinomas. In line with these facts, it is possible that activation of both the Wnt/β-catenin signaling pathway and the GTP-binding protein-mediated signaling pathway is associated with the development and progression of GA-FG. Further studies are needed to elucidate the histological characteristics of neoplastic progression and molecular changes in GA-FG.