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先天性肝内胆管错构瘤向肝内胆管癌肿瘤进展的组织病理学证据。

Histopathological evidence of neoplastic progression of von Meyenburg complex to intrahepatic cholangiocarcinoma.

作者信息

Bhalla Amarpreet, Mann Steven A, Chen Shaoxiong, Cummings Oscar W, Lin Jingmei

机构信息

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

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

出版信息

Hum Pathol. 2017 Sep;67:217-224. doi: 10.1016/j.humpath.2017.08.004. Epub 2017 Aug 18.

Abstract

Von Meyenburg complex (VMC) is generally thought to be benign, although its preneoplastic potential for intrahepatic cholangiocarcinoma (iCC) has been a subject of contention. We retrospectively reviewed 86 hepatectomy specimens with a diagnosis of iCC. Morphologically, an association between iCC and VMC was appreciated in 35% of cases that illustrated a gradual neoplastic progression from benign VMC to dysplasia and then to iCC. Among them, 24 cases had VMC lined by epithelial cells with low-grade biliary dysplasia and 13 with high-grade biliary dysplasia. VMC-associated iCCs were smaller in size and well to moderately differentiated, with features of anastomosing glandular architecture, ductal carcinoma in situ-like growth pattern, peritumoral lymphocytic infiltrate, central fibrous scar, and complete pushing border. They often presented as T1 tumors. In contrast, non-VMC-associated iCCs were moderately to poorly differentiated with solid, cribriform or papillary growth patterns. They likely exhibited necrosis, perineural invasion, positive surgical margin, lymphovascular invasion, and high T stage. Additionally, Ki67 and p53 immunostains support the continuing neoplastic evolution from benign VMC to dysplasia and then to iCC. VMC could become neoplastic, serving as an in situ carcinoma lesion to transform to iCC. The underlying molecular alteration and clinical implication of this neoplastic transformation deserves further investigation.

摘要

梅氏复合体(VMC)一般被认为是良性的,尽管其发生肝内胆管癌(iCC)的癌前潜能一直存在争议。我们回顾性分析了86例诊断为iCC的肝切除标本。形态学上,35%的病例显示iCC与VMC之间存在关联,呈现出从良性VMC逐渐发展为发育异常进而发展为iCC的肿瘤进展过程。其中,24例VMC内衬的上皮细胞有低级别胆管发育异常,13例有高级别胆管发育异常。与VMC相关的iCC体积较小,分化良好至中等,具有吻合性腺管结构、原位导管癌样生长模式、肿瘤周围淋巴细胞浸润、中央纤维瘢痕和完整的推挤边界等特征。它们常表现为T1期肿瘤。相比之下,与非VMC相关的iCC分化中等至较差,具有实性生长模式、筛状或乳头状生长模式。它们可能出现坏死、神经侵犯、手术切缘阳性、脉管侵犯和高T分期。此外,Ki67和p53免疫组化支持从良性VMC到发育异常再到iCC的持续肿瘤演变。VMC可能会发生肿瘤性变化,作为原位癌病灶转变为iCC。这种肿瘤转变的潜在分子改变和临床意义值得进一步研究。

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