Pathology of Hepatocellular Carcinoma and Tumor-Bearing Liver Tissue in Association with hTERT Promoter Mutation.

IF 1.5 Q3 GASTROENTEROLOGY & HEPATOLOGY International Journal of Hepatology Pub Date : 2023-08-09 eCollection Date: 2023-01-01 DOI:10.1155/2023/4313504
Anne Kristin Fischer, Alexander Semaan, Anna-Lena Wulf, Christian Vokuhl, Diane Goltz, Hans-Peter Fischer
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Abstract

Background: The hTERT promoter mutation represents a common and early event in hepatocarcinogenesis, but its linkage to the morphological status of the underlying liver tissue is poorly understood. We analyzed the connection between the histopathological changes in tumor-bearing liver tissue and the occurrence of the hTERT promoter mutation in hepatocellular carcinoma (HCC), correlated with clinical data.

Methods: The study cohort comprised 160 histologically confirmed HCC in patients with or without cirrhosis that were investigated for the hTERT promoter mutation. We evaluated the frequency of the hTERT promoter mutation in patients with HCC with or without cirrhosis and correlated it with potential clinical and histopathological drivers. In particular, we examined tumor-bearing noncirrhotic liver tissue regarding inflammation; the modified histological activity index (mHAI), fibrosis, and steatosis; and its correlation with the frequency of the hTERT promoter mutation in HCC. We evaluated overall survival with multivariate Cox regression. Furthermore, we compared hTERT antibody immunohistochemistry and molecular hTERT promoter mutation analysis of both HCC and background liver tissue.

Results: The hTERT promoter mutation was especially related to HCC in cirrhotic compared with noncirrhotic liver (p < 0.001) and independently of cirrhosis in patients ≥ 60 years (p = 0.005). Furthermore, the hTERT promoter mutation was associated with cirrhosis caused by alcohol toxicity and hepatitis C virus infection. In noncirrhotic liver tissue, the frequency of hTERT-promoter-mutated HCC increased with the degree of inflammation and fibrosis. Nevertheless, 25% of the hTERT-promoter-mutated HCC developed in normal liver tissue without HCC risk factors. Multivariate Cox regression analysis did not reveal an influence of the hTERT promoter mutation in HCC on overall survival at 3, 5, and 16 years. Immunohistochemical analysis with the hTERT antibodies LS-B95 and 2D8 in hTERT-promoter-mutated HCC and hTERT-wildtype HCC showed a mildly stronger immunoreaction compared with the tumor-bearing liver tissue (LS-B95: p < 0.01, 2D8: p < 0.01).

Conclusions: Our study reveals a connection between pathological changes in tumor-bearing liver tissue and the hTERT promoter mutation in most HCC, even in noncirrhotic liver tissue. Immunohistochemical hTERT antibodies do not discriminate between hTERT-promoter-mutated and wildtype HCC.

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与 hTERT Promoter 基因突变有关的肝细胞癌和带瘤肝组织病理学。
背景:hTERT启动子突变是肝癌发生过程中常见的早期事件,但人们对其与基础肝组织形态学状态的关系知之甚少。我们分析了肝细胞癌(HCC)中带瘤肝组织的组织病理学变化与 hTERT 启动子突变发生之间的联系,并将其与临床数据进行了关联分析:研究队列包括160例经组织学确诊的HCC患者,这些患者无论是否患有肝硬化,均接受了hTERT启动子突变的检查。我们评估了有肝硬化或无肝硬化的 HCC 患者中 hTERT 启动子突变的频率,并将其与潜在的临床和组织病理学驱动因素联系起来。特别是,我们检查了肿瘤携带的非肝硬化肝组织的炎症、改良组织学活性指数(mHAI)、纤维化和脂肪变性情况,及其与 HCC 中 hTERT 启动子突变频率的相关性。我们采用多变量考克斯回归法评估了总生存率。此外,我们还比较了HCC和背景肝组织的hTERT抗体免疫组化和分子hTERT启动子突变分析:结果:与非肝硬化患者相比,肝硬化患者的 hTERT 启动子突变与 HCC 尤为相关(p < 0.001),且与肝硬化无关(p = 0.005)。此外,hTERT启动子突变与酒精中毒和丙型肝炎病毒感染导致的肝硬化有关。在非肝硬化肝组织中,hTERT启动子突变的HCC频率随着炎症和纤维化程度的增加而增加。然而,25%的hTERT突变型HCC发生在无HCC风险因素的正常肝组织中。多变量Cox回归分析并未显示HCC中的hTERT启动子突变对3年、5年和16年的总生存率有影响。用hTERT启动子突变的HCC和hTERT野生型HCC中的hTERT抗体LS-B95和2D8进行免疫组化分析显示,与肿瘤肝组织相比,免疫反应轻微增强(LS-B95:p < 0.01,2D8:p < 0.01):我们的研究揭示了大多数 HCC(即使是非肝硬化肝组织)中带瘤肝组织的病理变化与 hTERT 启动子突变之间的联系。免疫组化 hTERT 抗体不能区分 hTERT 启动子突变和野生型 HCC。
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来源期刊
International Journal of Hepatology
International Journal of Hepatology GASTROENTEROLOGY & HEPATOLOGY-
CiteScore
3.80
自引率
0.00%
发文量
11
审稿时长
15 weeks
期刊介绍: International Journal of Hepatology is a peer-reviewed, Open Access journal that publishes original research articles, review articles, and clinical studies related to the medical, surgical, pathological, biochemical, and physiological aspects of hepatology, as well as the management of disorders affecting the liver, gallbladder, biliary tree, and pancreas.
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