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CDX2、细胞角蛋白7和20在直肠腺癌中的免疫反应性。

CDX2, cytokeratins 7 and 20 immunoreactivity in rectal adenocarcinoma.

作者信息

Saad Reda S, Silverman Jan F, Khalifa Mahmoud A, Rowsell Corwyn

机构信息

Department of Pathology, Sunnybrook Health Science Center, University of Toronto, Toronto, Ontario, Canada.

出版信息

Appl Immunohistochem Mol Morphol. 2009 May;17(3):196-201. doi: 10.1097/PAI.0b013e31819268f2.

Abstract

There are limited data regarding CDX2 expression in rectal carcinoma. The CK20/CK7 immunoprofile of colorectal adenocarcinoma has been described in studies, which have mostly lumped colonic and rectal tumors together. In this study, we investigated the diagnostic utility of immunohistochemical stains for CK7, CK20, and CDX2 in a series of rectal adenocarcinoma. Fifty-five specimens of rectal adenocarcinomas were retrieved and immunostained for CK7 (Dako-M7018), CK20 (NovoCastra NCL-L-CK20), and CDX2 (NovoCastra NCL-CDX2). Thirty cases of pancreatic adenocarcinoma and 15 cholangiocarcinomas were also studied as a comparison group. CK7 was expressed in 12/55 (22%) and CK20 in 48/55 (87%) cases of rectal adenocarcinoma. The CK7-/CK20+ immunophenotype was identified in 36/55 (65%), CK7+/CK20+ in 12/55 (22%), and CK7-/CK20- in 7/55 (13%) rectal adenocarcinoma. CDX2 showed moderate-strong positivity in all cases and was not related to tumor differentiation. Benign rectal mucosa was available in 37 cases and showed the following results: CK7-/CK20+ in 25/37 (67%), CK7+/CK20+ in 8/37 (22%) and CK7-/CK20- in 4/37 (11%) cases. In pancreatic adenocarcinomas and cholangiocarcinomas, 29/45 (64%) were CK7+/CK20+ and 16/45 (36%) were CK7+/CK20-. CDX2 was positive in only 3/45 (7%) of these cases; all were pancreatic adenocarcinomas. In conclusion, CK7 can be expressed in rectal adenocarcinoma, and should not be used as the sole basis for excluding a rectal primary. CDX2 is a sensitive marker for rectal origin of adenocarcinoma. It can be helpful in cases with metastatic rectal carcinoma, especially those with CK7+/CK20+ or CK20-/CK7- immunophenotype. In this study, CDX2 expression was not influenced by the grade (differentiation) of rectal adenocarcinoma.

摘要

关于CDX2在直肠癌中的表达数据有限。结直肠癌的CK20/CK7免疫表型已在研究中有所描述,但这些研究大多将结肠和直肠肿瘤合并在一起。在本研究中,我们调查了免疫组化染色检测CK7、CK20和CDX2在一系列直肠腺癌中的诊断效用。收集了55例直肠腺癌标本,并对其进行CK7(Dako-M7018)、CK20(NovoCastra NCL-L-CK20)和CDX2(NovoCastra NCL-CDX2)免疫染色。还研究了30例胰腺腺癌和15例胆管癌作为对照组。在55例直肠腺癌中,12例(22%)表达CK7,48例(87%)表达CK20。55例直肠腺癌中,36例(65%)为CK7-/CK20+免疫表型,12例(22%)为CK7+/CK20+,7例(13%)为CK7-/CK20-。所有病例中CDX2均呈中度至强阳性,且与肿瘤分化无关。有37例可获得良性直肠黏膜,结果如下:25例(67%)为CK7-/CK20+,8例(22%)为CK7+/CK20+,4例(11%)为CK7-/CK20-。在胰腺腺癌和胆管癌中,29例(64%)为CK7+/CK20+,16例(36%)为CK7+/CK20-。这些病例中只有3例(7%)CDX2呈阳性;均为胰腺腺癌。总之,CK7可在直肠腺癌中表达,不应作为排除直肠原发肿瘤的唯一依据。CDX2是腺癌直肠起源敏感的标志物。它对转移性直肠癌病例有帮助,尤其是那些具有CK7+/CK20+或CK20-/CK7-免疫表型的病例。在本研究中,CDX2表达不受直肠腺癌分级(分化)的影响。

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