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通过基于尸检的全基因组微卫星分析评估肝细胞癌的基因型稳定性和克隆进化。

Genotype stability and clonal evolution of hepatocellular carcinoma assessed by autopsy-based genome-wide microsatellite analysis.

作者信息

Nishimura Takafumi, Nishida Naoshi, Komeda Toshiki, Fukuda Yoshihiro, Nakao Kazuwa

机构信息

Department of Medicine and Clinical Science, Kyoto University Graduate School of Medicine, 54 Kawahara-cho, Shogoin, Sakyo-ku, Kyoto 606-8507, Japan.

出版信息

Cancer Genet Cytogenet. 2005 Sep;161(2):164-9. doi: 10.1016/j.cancergencyto.2005.02.011.

Abstract

It is widely accepted that chromosomal instability is an essential feature of cancer cells including hepatocellular carcinoma (HCC) cells. For an accurate characterization of clonal evolution of HCC cells, we studied chromosomal alterations in various metastatic lesions in an autopsy case of HCC. Tissues from the main tumor, which consisted of 2 macroscopically distinct portions, and from intrahepatic metastasis, portal vein thrombus, epiploic lymph node metastasis, and pulmonary metastasis as well as from the non-tumorous liver were analyzed with comprehensive microsatellite analysis. Alleles showing imbalance of the main tumor were further subjected to comparative duplex PCR, with use of a retained allele as an internal control, to determine whether the imbalance was the result of chromosomal gain or loss. A striking finding was that allelic imbalances detected in the main tumor and metastatic lesions were almost identical, showing -1p, +1q, -4q, -7, -8p, +8q, +9q, +10, -13q, -17p, +19p, -19q, and -X. Additional alterations of +2q and -16q were detected in one portion of the main tumor and the portal vein thrombus. In conclusion, clonal evolution of the HCC cells during metastatic progression seems rare, in contrast to many recurrent chromosomal aberrations that may have accumulated before the clinical manifestation.

摘要

人们普遍认为,染色体不稳定是包括肝癌(HCC)细胞在内的癌细胞的一个基本特征。为了准确表征HCC细胞的克隆进化,我们在一例HCC尸检病例中研究了各种转移病灶中的染色体改变。对主要肿瘤(由两个宏观上不同的部分组成)、肝内转移灶、门静脉血栓、网膜淋巴结转移灶、肺转移灶以及非肿瘤性肝脏的组织进行了全面的微卫星分析。对显示主要肿瘤不平衡的等位基因进一步进行比较双链PCR,以保留的等位基因为内部对照,确定这种不平衡是染色体增加还是减少的结果。一个惊人的发现是,在主要肿瘤和转移病灶中检测到的等位基因不平衡几乎相同,表现为-1p、+1q、-4q、-7、-8p、+8q、+9q、+10、-13q、-17p、+19p、-19q和-X。在主要肿瘤的一部分和门静脉血栓中检测到+2q和-16q的额外改变。总之,与许多可能在临床表现之前就已积累的反复出现的染色体畸变相反,HCC细胞在转移过程中的克隆进化似乎很少见。

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