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细胞角蛋白19和细胞角蛋白7在发育异常结节及肝细胞癌中的表达

Expression of K19 and K7 in dysplastic nodules and hepatocellular carcinoma.

作者信息

Bae Jun Sang, Choi Ha Na, Noh Sang Jae, Park Byung Hyun, Jang Kyu Yun, Park Cheol Keun, Moon Woo Sung

机构信息

Department of Pathology, Chonbuk National University, Medical School and Research Institute for Endocrine Sciences, Jeonju, 561-756.

出版信息

Oncol Lett. 2012 Aug;4(2):213-220. doi: 10.3892/ol.2012.731. Epub 2012 May 25.

Abstract

Hepatocellular carcinoma (HCC) is one of the most common types of malignant tumors characterized by a multistep process of tumor development. Nodular lesions that differ from the surrounding liver parenchyma and are characterized by cytological or structural atypia are termed dysplastic nodules (DNs). DNs are well-known precancerous HCC lesions. Expression of keratin (K) 19 and K7, molecular markers of hepatic progenitor cells and cholangiocytes, has been reported in certain HCCs. However, it remains unclear whether K19-positive HCC cells are derived from true hepatic progenitor cells or mature cells that have undergone a dedifferentiation or a transdifferentiation process. In total, 107 tissue sections (13 low-grade DNs, 15 high-grade DNs, 27 small HCCs and 52 large HCCs) from resected liver samples and 132 HCC tissue microarray (TMA) cores were subjected to immunohistochemical analysis for K19 and K7. Clinicopathological data of the HCC patients were evaluated. K19 expression was found in 0% of DNs, 19% of small HCCs (≤2 cm), 8% of large HCCs (>2 cm) and 8% of TMA samples. K7 expression was found in 14% of DNs, 41% of small HCCs, 15% of large HCCs and 6% of TMA samples. Among the five K19-positive small HCCs, four were distinctly nodular and one tumor was an infiltrative type. No vaguely nodular HCC was positive for K19. K19 expression was significantly associated with histological grade (P=0.023), serum α-fetoprotein level (P=0.001) and K7 expression (P=0.001) in HCC. K19 expression was an independent prognostic factor for overall survival in non-viral HCC patients (P=0.003). K19 expression is extremely rare in DNs and occurs in progressed small HCCs. Our results suggest that K19 expression may be an acquired feature of carcinoma cells during HCC progression in certain HCCs.

摘要

肝细胞癌(HCC)是最常见的恶性肿瘤类型之一,其特征为肿瘤发展的多步骤过程。与周围肝实质不同且具有细胞学或结构异型性的结节性病变被称为发育异常结节(DNs)。DNs是众所周知的HCC癌前病变。在某些HCC中已报道了肝祖细胞和胆管细胞的分子标志物角蛋白(K)19和K7的表达。然而,K19阳性的HCC细胞是源自真正的肝祖细胞还是经历了去分化或转分化过程的成熟细胞仍不清楚。对来自切除肝脏样本的107个组织切片(13个低级别DNs、15个高级别DNs、27个小HCC和52个大HCC)以及132个HCC组织微阵列(TMA)核心进行K19和K7的免疫组织化学分析。评估了HCC患者的临床病理数据。在DNs中K19表达为0%,在小HCC(≤2 cm)中为19%,在大HCC(>2 cm)中为8%,在TMA样本中为8%。在DNs中K7表达为14%,在小HCC中为41%,在大HCC中为15%,在TMA样本中为6%。在五个K19阳性的小HCC中,四个为明显结节性,一个肿瘤为浸润型。没有模糊结节性HCC为K19阳性。在HCC中,K19表达与组织学分级(P=0.023)、血清甲胎蛋白水平(P=0.001)和K7表达(P=0.001)显著相关。K19表达是无病毒HCC患者总生存的独立预后因素(P=0.003)。K19表达在DNs中极为罕见,且发生于进展期小HCC中。我们的结果表明,在某些HCC中,K19表达可能是HCC进展过程中癌细胞的一种获得性特征。

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