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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.
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