基于 U-P 点划分的肝周胆管癌病理学和分子特征

Ying Xiao, Qijia Zhang, Canhong Xiang, Jianghui Yang, Bowen Li, Hongfang Yin
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引用次数: 0

摘要

背景:日本肝胆胰外科协会指南提出了一种不同于国际癌症控制联盟(UICC)系统的分类方案,在该系统中,解剖学U-P点是肝内胆管癌和肝周胆管癌(PCC)的分界线:研究该分类系统是否能改善临床病理和基因组分化:收集了58例由UICC系统定义的PCC病例,并采用U-P点划分法将其分为肝内PCC(IPCC)和肝外PCC(EPCC)两类。通过使用针对 425 个癌症相关基因的面板进行下一代测序,对这些病例进行了分析:IPCC组的肿瘤大小明显大于EPCC组(4.67 ± 2.44 cm对2.50 ± 0.91 cm,P = .002)。IPCC 组 KRAS 原癌基因 GTPase(KRAS)Q61 的突变频率也明显高于 EPCC 组(16.7% 对 0.0%,P = .03)。其他病理特征或基因组特征(包括肿瘤突变负荷和微卫星不稳定性)无统计学差异。在基因突变率方面,如磷脂酰肌醇-4,5-二磷酸 3-激酶催化亚基α(PIK3CA;0.0% 对 15.8%,P = .01)和肿瘤蛋白 p53(TP53;34.5% 对 63.2%,P = .04),PCC 与邻近胆道癌之间存在显著差异:本研究为了解 PCC 的临床病理和基因组特征提供了宝贵的信息。结论:本研究对 PCC 的临床病理和基因组特征提供了有价值的见解,并提出 U-P 点划分在完善 PCC 这些特征方面的潜力可能有限,而 UICC 分类系统可轻松证明 PCC 的分子特异性。
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Pathologic and Molecular Features of Perihilar Cholangiocarcinoma Based on U-P Point Division.

Context.—: The Japanese Society of Hepato-Biliary-Pancreatic Surgery guidelines propose a classification scheme that differs from the Union for International Cancer Control (UICC) system, in which the anatomic U-P point is the boundary between intrahepatic cholangiocarcinoma and perihilar cholangiocarcinoma (PCC).

Objective.—: To investigate whether this classification system improves clinicopathologic and genomic differentiation.

Design.—: Fifty-eight PCC cases defined by the UICC system were collected and classified into intrahepatic PCC (IPCC) and extrahepatic PCC (EPCC) categories using U-P point division. They were analyzed by next-generation sequencing using a panel that targeted 425 cancer-related genes.

Results.—: The IPCC group exhibited a significant larger tumor size compared with the EPCC group (4.67 ± 2.44 cm versus 2.50 ± 0.91 cm, P = .002). The mutation frequency of KRAS proto-oncogene, GTPase (KRAS) Q61 was also significantly higher in the IPCC group than in the EPCC group (16.7% versus 0.0%, P = .03). There were no statistically significant differences in other pathologic features or genomic characteristics, including tumor mutation burden and microsatellite instability. Significant differences in gene mutation rates, such as phosphatidylinositol-4,5-bisphosphate 3-kinase catalytic subunit alpha (PIK3CA; 0.0% versus 15.8%, P = .01) and tumor protein p53 (TP53; 34.5% versus 63.2%, P = .04), were observed between PCC and adjacent biliary tract cancers.

Conclusions.—: This study offers valuable insight into the clinicopathologic and genomic features of PCC. It is proposed that the U-P point division may have limited potential to refine the characterization of PCC regarding these features, and that the UICC classification system can readily demonstrate the molecular specificity of PCC.

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