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胃腺癌和近端息肉病综合征(GAPPS)的肿瘤性病变为胃表型。

Neoplastic Lesions of Gastric Adenocarcinoma and Proximal Polyposis Syndrome (GAPPS) Are Gastric Phenotype.

作者信息

de Boer Willem B, Ee Hooi, Kumarasinghe Marian P

机构信息

PathWest Laboratory Medicine (QE 2 Medical Centre) and University of Western Australia.

Department of Gastroenterology, Sir Charles Gairdner Hospital, Perth, WA, Australia.

出版信息

Am J Surg Pathol. 2018 Jan;42(1):1-8. doi: 10.1097/PAS.0000000000000924.

DOI:10.1097/PAS.0000000000000924
PMID:29112017
Abstract

UNLABELLED

Neoplastic lesions of gastric adenocarcinoma and proximal polyposis of the stomach (GAPPS) are gastric phenotype. GAPPS was reported in 2011 as a new autosomal dominant gastric polyposis syndrome characterized by involvement of the gastric body/fundus with sparing of the antrum by multiple polyps, reported to be primarily fundic gland polyps (FGPs), with progression to dysplasia and adenocarcinoma of intestinal type. Our series consists of 51 endoscopic biopsies and 5 gastrectomy specimens from 25 patients belonging to a previously defined GAPPS family. Slides were reviewed and further stains performed. Endoscopy was abnormal in 15 of the 25 patients: carpeting polyposis of the gastric body and fundus in 14 and a gastric mass without polyposis in one. The most common polypoid lesion (seen in 12 patients) was a disorganized proliferation of specialized/oxyntic glands high up in the mucosa involving the attenuated foveolar region around the gastric pits, which we have termed "hyperproliferative aberrant pits". Well developed FGP were seen in 10 patients. Established neoplastic lesions seen in 9 patients were: (1) discrete gastric adenomas, (2) multifocal "flat" dysplasia in the setting of hyperproliferative aberrant pits +/- FGPs, (3) adenomatous tissue associated with adenocarcinoma. All cases of dysplasia were of gastric phenotype based on morphology and mucin immunohistochemistry.

IN CONCLUSION

(1) the spectrum of gastric pathology associated with GAPPS is wider than previously reported, (2) the earliest microscopic clue is the finding of hyperproliferative aberrant pits, and (3) the dysplasia is gastric phenotype and the subsequent adenocarcinoma may follow the gastric pathway of carcinogenesis.

摘要

未标记

胃腺癌和胃近端息肉病(GAPPS)的肿瘤性病变具有胃表型。GAPPS于2011年被报道为一种新的常染色体显性遗传胃息肉病综合征,其特征为胃体/胃底受累,胃窦部无息肉,据报道主要为胃底腺息肉(FGP),可进展为异型增生和肠型腺癌。我们的系列研究包括来自一个先前定义的GAPPS家族的25例患者的51份内镜活检标本和5份胃切除标本。对切片进行了复查并进行了进一步染色。25例患者中有15例内镜检查异常:14例为胃体和胃底的地毯样息肉病,1例为无息肉的胃肿物。最常见的息肉样病变(见于12例患者)是黏膜高处特殊/泌酸腺的无序增生,累及胃小凹周围变薄的小凹区域,我们将其称为“增生异常的小凹”。10例患者可见发育良好的FGP。9例患者中发现的已确诊肿瘤性病变为:(1)离散性胃腺瘤,(2)增生异常的小凹±FGP背景下的多灶性“扁平”异型增生,(3)与腺癌相关的腺瘤组织。根据形态学和黏液免疫组化,所有异型增生病例均为胃表型。

结论

(1)与GAPPS相关的胃病理学范围比先前报道的更广,(2)最早的微观线索是发现增生异常的小凹,(3)异型增生为胃表型,随后的腺癌可能遵循胃癌发生的胃途径。

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