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膀胱肠化生和腺性膀胱炎的不同发展途径。

Divergent pathway of intestinal metaplasia and cystitis glandularis of the urinary bladder.

作者信息

Sung Ming-Tse, Lopez-Beltran Antonio, Eble John N, MacLennan Gregory T, Tan Puay-Hoon, Montironi Rodolfo, Jones Timothy D, Ulbright Thomas M, Blair Jean E, Cheng Liang

机构信息

Department of Pathology and Laboratory Medicine, Indiana University School of Medicine, Indianapolis, IN 46202, USA.

出版信息

Mod Pathol. 2006 Nov;19(11):1395-401. doi: 10.1038/modpathol.3800670. Epub 2006 Sep 1.

Abstract

Intestinal metaplasia has been proposed to be a precursor lesion of adenocarcinoma in the urinary bladder. CDX2 is a transcription factor that is encoded by a homeotype gene that plays an essential role in the differentiation and proliferation of intestinal epithelial cells. Hepatocyte-specific antigen (Hep) has also been shown to be a useful marker of intestinal metaplasia. Tissues from 46 patients, including 22 cases of intestinal metaplasia of the urinary bladder, 11 cases of typical cystitis glandularis, and 13 cases containing both lesions, were selected and immunohistochemical stains for CDX2, Hep, cytokeratin 20 (CK20), and cytokeratin 7 (CK7) were performed. Nuclear staining for CDX2 was observed in 29 of 35 (83%) cases of intestinal metaplasia of the urinary bladder. In contrast, nuclear staining for CDX2 was not observed in any case of typical cystitis glandularis; however, seven of 24 (29%) cases showed aberrant cytoplasmic expression in a mean of 37% of cells. CK20 was expressed in 28 of 35 (80%) cases of intestinal metaplasia, but was observed in only one of 24 (4%) cases of cystitis glandularis in 15% of cells. CK7 was expressed in only six of 35 (17%) cases of intestinal metaplasia, whereas expression of CK7 was observed in all cases (100%) of typical cystitis glandularis with a mean percentage of positively staining cells of 63%. The mean percentages of positively staining cells in intestinal metaplasia with CDX2, CK20, and CK7 were 55, 49, and 53%, respectively. All examples of both intestinal metaplasia and typical cystitis glandularis were uniformly negative for Hep. In the urinary bladder, intestinal metaplasia and typical cystitis glandularis have sharply contrasting immunoprofiles. Additionally, the absence of Hep staining in intestinal metaplasia of the urinary bladder, despite its morphologic resemblance to normal colonic mucosa and intestinal metaplasia in other organs, may signify the presence of unique metaplastic pathways in the urinary bladder.

摘要

肠化生被认为是膀胱腺癌的一种前驱病变。CDX2是一种转录因子,由一个同源异型基因编码,该基因在肠道上皮细胞的分化和增殖中起重要作用。肝细胞特异性抗原(Hep)也已被证明是肠化生的一个有用标志物。选取了46例患者的组织,包括22例膀胱肠化生、11例典型腺性膀胱炎以及13例同时含有这两种病变的组织,并对CDX2、Hep、细胞角蛋白20(CK20)和细胞角蛋白7(CK7)进行免疫组织化学染色。在35例膀胱肠化生病例中的29例(83%)观察到CDX2的核染色。相比之下,在任何典型腺性膀胱炎病例中均未观察到CDX2的核染色;然而,24例中的7例(29%)在平均37%的细胞中显示异常的细胞质表达。CK20在35例膀胱肠化生病例中的28例(80%)中表达,但在24例腺性膀胱炎病例中仅1例(4%)在15%的细胞中观察到表达。CK7仅在35例膀胱肠化生病例中的6例(17%)中表达,而在所有典型腺性膀胱炎病例(100%)中均观察到CK7表达,阳性染色细胞的平均百分比为63%。CDX2、CK20和CK7在肠化生中阳性染色细胞的平均百分比分别为55%、49%和53%。肠化生和典型腺性膀胱炎的所有样本Hep均呈一致阴性。在膀胱中,肠化生和典型腺性膀胱炎具有截然不同的免疫表型。此外,膀胱肠化生中尽管其形态与正常结肠黏膜及其他器官的肠化生相似,但Hep染色缺失,这可能表明膀胱中存在独特的化生途径。

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