Abstract
BackgroundCrawling-type adenocarcinoma (CRA) is an important gastric cancer (GC) subtype that exhibits a specific histological pattern and has characteristic clinicopathological findings. Despite its characteristic histology, little is known about the molecular characteristics of CRA.MethodsWe examined 177 GC cases, including 51 cases of CRA and 126 cases having conventional differentiated adenocarcinomas (CDAs). Results for immunohistochemistry (mucin phenotype; Muc5AC, Muc6, Muc2 and CD10, CDX-2, MLH-1, p53 and β-catenin), mutation analysis (TP53, KRAS and BRAF), microsatellite instability (BAT25, BAT26, D2S123, D5S346 and D17S250), DNA methylation status by a two-panel method (RUNX3, MINT31, LOX, NEUROG1, ELMO1 and THBD), MLH-1 promoter methylation, and allelic imbalance (AI; 1p, 3p, 4p, 5q, 8p, 9p, 13q, TP53, 18q and 22q) were examined.ResultsCRAs were more likely to occur in the middle third of the stomach, in younger patients and to be macroscopically depressed. Nuclear accumulation of β-catenin and loss of MLH-1 expression were less frequent among CRA cases compared to CDA cases. At a molecular level, CRA is often characterized by the deletion mutation c.529_546 (18-base pair deletion at codon 177–182 in exon 5) in the TP53 gene (10 cases). Although the low methylation epigenotype was significantly more frequent for CRAs compared to CDAs, multiple AIs were more often seen in CRAs relative to CDAs.ConclusionsThe results demonstrated that TP53 mutations, particularly c.529_546del, and multiple AIs are closely associated with CRA carcinogenesis. Our results suggest that CRA is an independent entity of GC in terms of clinicopathologic and molecular findings.
Highlights
Crawling-type adenocarcinoma (CRA) is an important gastric cancer (GC) subtype that exhibits a specific histological pattern and has characteristic clinicopathological findings
CRAs were more frequently localized in the middle third of the stomach than were conventional differentiated adenocarcinoma (CDA) (CRA, 32/51, 62.8%; CDA, 46/ 126, 36.5%; P < 0.01)
Depressed type tumors were significantly more frequent in CRA compared to CDA (37/ 51, 72.5% vs. 46/126, 36.5%; P < 0.01)
Summary
Crawling-type adenocarcinoma (CRA) is an important gastric cancer (GC) subtype that exhibits a specific histological pattern and has characteristic clinicopathological findings. Crawling-type adenocarcinoma (CRA) is an important subtype among moderately-differentiated adenocarcinomas and has attracted increased attention as a specific histological GC subtype due to its characteristic clinicopathological and molecular findings [3,4,5,6]. Cancer glands in CRA show a complex architecture described as a “shaking-hands pattern” or “WHYX pattern” [5, 7], due to subtle cytological atypia such tumor glands can appear to be an “intestinal metaplasia” that is a benign lesion. Distinguishing this type of GC from non-neoplastic lesions, such as intestinal metaplasia, can be challenging
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