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关于肝细胞癌转移的十年研究。

A decade's studies on metastasis of hepatocellular carcinoma.

作者信息

Tang Zhao-You, Ye Sheng-Long, Liu Yin-Kun, Qin Lun-Xiu, Sun Hui-Chuan, Ye Qin-Hai, Wang Lu, Zhou Jian, Qiu Shuang-Jian, Li Yan, Ji Xue-Ning, Liu Hu, Xia Jing-Ling, Wu Zhi-Quan, Fan Jia, Ma Zeng-Chen, Zhou Xin-Da, Lin Zhi-Ying, Liu Kang-Da

机构信息

Liver Cancer Institute, Zhongshan Hospital, 136 Yi Xue Yuan Road, 200032, Shanghai, PR China.

出版信息

J Cancer Res Clin Oncol. 2004 Apr;130(4):187-96. doi: 10.1007/s00432-003-0511-1. Epub 2003 Dec 18.

Abstract

Metastasis remains one of the major challenges before hepatocellular carcinoma (HCC) is finally conquered. This paper summarized a decade's studies on HCC metastasis at the Liver Cancer Institute of Fudan University. We have established a stepwise metastatic human HCC model system, which included a metastatic HCC model in nude mice (LCI-D20), a HCC cell line with high metastatic potential (MHCC97), a relatively low metastatic potential cell clone (MHCC97L) and several stepwise high metastatic potential cell clones (MHCC97H, HCCLM3, and HCCLM6) from their parent MHCC97 cell. Endeavors have been made for searching human HCC metastasis-related chromosomes/proteins/genes. Monogene-based studies revealed that HCC invasion/metastasis was similar to that of other solid tumors, and the biological characteristics of small HCC were only slightly better than that of large HCC. Using comparative genomic hybridization (CGH), fluorescence in situ hybridization (FISH), genotyping, cDNA microarray, and 2-dimensional gel electrophoresis, we obtained some interesting results. In particular, in collaboration with the National Institute of Health (NIH) in the United States, we generated a molecular signature that can classify metastatic HCC patients, identified osteopontin as a lead gene in the signature, and found that genes favoring metastasis progression were initiated in the primary tumors. We also found that chromosome 8p deletion, particularly in the region of 8p23, was associated with HCC metastasis. Cytokeratin 19 was identified as one of the proteins, which was found in MHCC97H, but not in MHCC97L cells. Experimental interventions using the high metastatic nude mice model have provided clues for the prevention of HCC metastasis. Translation from workbench to bedside demonstrated that serum VEGF, microvessel density, and p53 scoring may be of value for the prediction of postoperative metastatic recurrence. Interferon alpha proved effective for the prevention of recurrence both experimentally and clinically. In conclusion, HCC metastasis that probably initiated in the primary tumor is a multigene-involved, multistep, and changing process. The further elucidation of the mechanism underlying HCC metastasis will provide a more solid basis for the prediction and prevention of the metastatic recurrence of HCC.

摘要

在肝细胞癌(HCC)最终被攻克之前,转移仍然是主要挑战之一。本文总结了复旦大学肝癌研究所对HCC转移的十年研究。我们建立了一个逐步转移的人HCC模型系统,其中包括裸鼠体内的转移HCC模型(LCI-D20)、具有高转移潜能的HCC细胞系(MHCC97)、转移潜能相对较低的细胞克隆(MHCC97L)以及从其亲本MHCC97细胞衍生而来的几个逐步具有高转移潜能的细胞克隆(MHCC97H、HCCLM3和HCCLM6)。我们致力于寻找与人类HCC转移相关的染色体/蛋白质/基因。基于单基因的研究表明,HCC的侵袭/转移与其他实体瘤相似,小HCC的生物学特性仅略优于大HCC。通过比较基因组杂交(CGH)、荧光原位杂交(FISH)、基因分型、cDNA微阵列和二维凝胶电泳,我们获得了一些有趣的结果。特别是,与美国国立卫生研究院(NIH)合作,我们生成了一个可对转移性HCC患者进行分类的分子特征,确定骨桥蛋白为该特征中的主导基因,并发现促进转移进展的基因在原发性肿瘤中就已启动。我们还发现8号染色体短臂缺失,尤其是在8p23区域,与HCC转移相关。细胞角蛋白19被确定为一种蛋白质,在MHCC97H细胞中存在,但在MHCC97L细胞中不存在。使用高转移裸鼠模型进行的实验干预为预防HCC转移提供了线索。从实验室到临床的转化研究表明,血清血管内皮生长因子(VEGF)、微血管密度和p53评分可能对预测术后转移复发有价值。实验和临床研究均证明,α干扰素对预防复发有效。总之,可能始于原发性肿瘤的HCC转移是一个涉及多基因、多步骤且不断变化的过程。进一步阐明HCC转移的机制将为预测和预防HCC转移复发提供更坚实的基础。

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