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混合低级别和高级别乳头状尿路上皮癌:组织病理发生学和临床意义。

Mixed low- and high-grade papillary urothelial carcinoma: histopathogenetic and clinical significance.

机构信息

Department of Pathology and Laboratory Medicine, The Ottawa Hospital, University of Ottawa, Ottawa, Ontario, Canada,

出版信息

Virchows Arch. 2013 Oct;463(4):575-81. doi: 10.1007/s00428-013-1456-7. Epub 2013 Aug 4.

Abstract

There are two pathways of urothelial carcinogenesis: low-grade urothelial carcinoma (LGUC) with low rates of gene alterations and high-grade urothelial carcinoma (HGUC) with numerous gene alterations. HGUC often displays strong reactivity for cytokeratin 20 (CK20) and p16. Despite distinct molecular changes, urothelial carcinoma (UC) with both low- and high-grade features is not uncommon. We examined cases with patterns of mixed low- and high-grade UC (MLHGUC). Consecutive cases of UC at our institution were reviewed. There were 45 cases that showed a mixture of both LGUC and HGUC. IHC for CK5, CK20, CD44, p16, and Ki67 was performed. Areas of HGUC displayed strong and diffuse reactivity for p16, CK20, and Ki67 in 20-50 % of the tumor, while LGUC areas had negative or focal reactivity for CK20 and Ki67 in 10-30 %. There were two distinct cohorts of MLHGUC: patients with a history of LGUC (group A) and those without (group B). Group A patients (n = 8) had a history of LGUC for 1-10 years. The tumor specimens weighed 1.5 ± 1.7 g and had HGUC components of 25 ± 20 % of the tissue. Superficial invasion was present in one case. All tumors had BCG treatment with one recurrence. In group B (n = 37), tumor specimens weighed 3 ± 3.9 g and had HGUC components in 43 ± 21 % of the tissue. Superficial invasion was present in five cases, and muscle invasion with lung metastasis occurred in one case. Four cases were refractory to BCG with an increased proportion of HGUC, and one case requiring cystectomy. Differences in size and proportion of HGUC between groups A and B MLHGUC were significant (P < 0.05), with group B presenting with a higher tumor burden and proportion of HGUC. MLHGUC is diagnostically challenging and is commonly assigned high grade since this determines prognosis. Group A MLHGUC likely develops as a result of progression from LGUC, whereas group B MLHGUC likely develops de novo, is associated with larger tumors, shows a higher proportion of HGUC, and follows a worse prognosis. Despite the similar histology of groups A and B, assignment to HGUC in a binary system may mask important prognostic information.

摘要

有两种尿路上皮癌的发生途径

低级别尿路上皮癌(LGUC),其基因改变率较低,高级别尿路上皮癌(HGUC),其基因改变率较高。HGUC 通常对细胞角蛋白 20(CK20)和 p16 显示强烈的反应。尽管存在明显的分子变化,但具有低级别和高级别特征的尿路上皮癌(UC)并不少见。我们检查了具有混合低级别和高级别 UC(MLHGUC)模式的病例。对我院连续病例进行了回顾性研究。有 45 例病例显示 LGUC 和 HGUC 混合存在。对 CK5、CK20、CD44、p16 和 Ki67 进行了免疫组化染色。HGUC 区域的 p16、CK20 和 Ki67 在肿瘤的 20-50%呈强烈弥漫性反应,而 LGUC 区域的 CK20 和 Ki67 在 10-30%呈阴性或局灶性反应。MLHGUC 有两个明显的队列:有 LGUC 病史的患者(A 组)和无 LGUC 病史的患者(B 组)。A 组患者(n=8)有 1-10 年的 LGUC 病史。肿瘤标本重 1.5±1.7g,组织中有 25±20%的 HGUC 成分。1 例存在浅层浸润。所有肿瘤均接受 BCG 治疗,其中 1 例复发。B 组(n=37)肿瘤标本重 3±3.9g,组织中 HGUC 成分占 43±21%。5 例存在浅层浸润,1 例发生肌肉浸润和肺转移。4 例对 BCG 耐药,HGUC 比例增加,1 例需要行膀胱切除术。A、B 两组 MLHGUC 在肿瘤大小和 HGUC 比例方面存在显著差异(P<0.05),B 组肿瘤负荷和 HGUC 比例较高。MLHGUC 的诊断具有挑战性,由于其决定预后,通常被归为高级别。A 组 MLHGUC 可能是由 LGUC 进展而来,而 B 组 MLHGUC 可能是从头发生的,与较大的肿瘤相关,HGUC 比例较高,预后较差。尽管 A 组和 B 组的组织学相似,但在二元系统中归入 HGUC 可能会掩盖重要的预后信息。

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