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在裸鼠中鉴定与人类实验性结肠癌肝转移过程相关的基因改变。

Identification of genetic alterations associated with the process of human experimental colon cancer liver metastasis in the nude mouse.

作者信息

Yeatman T J, Cher M L, Mao W, Wloch M, Tedesco T

机构信息

H. Lee Moffitt Cancer Center & Research Institute, University of South Florida, Tampa, FL, USA.

出版信息

Clin Exp Metastasis. 1996 May;14(3):246-52. doi: 10.1007/BF00053898.

Abstract

Understanding the genetic elements controlling the process of tumor metastasis to distant organ sites such as the liver may be the key to improving survivorship from colon cancer. By using standard cytogenetic techniques in combination with comparative genomic hybridization, multiple genetic imbalances within three human colon cancer cell lines previously selected for differences in liver-metastatic behavior were identified. The entire genome of one poorly metastatic cell line (KM12C) was compared directly with that of two highly metastatic cell lines (KM12SM, KM12L4A) derived from it. A number of chromosomal gains (8q, 12q15, 20q11.2) and losses (5p13, 6p21.3, 18) were common to all three cell lines and are likely related to early tumor development rather than to the selection process used to generate cell lines of increased metastatic potential. Chromosomal imbalances detected only in the highly metastatic cell lines were also observed. KM12SM showed losses of portions of 2p22, 2q24.3--> 2q32.2, 4p15.3--> cen, 4q24 without the 13q and 15q22.3 gains noted for KM12C. Both gains (1p31.3--> 1p21, 2q22--> 2q33, 3cen--> 3q26.2, 5q14--> 5q23, 6cen--> 6q23) and losses (16p, 17p, 17q 19p, 19q 22q) were observed for KM12L4A but not for the other two cell lines. Identification of these alterations provides valuable insight into the process of experimental liver metastasis and is a first step towards mapping genes linked to the terminal phases of human colon cancer progression.

摘要

了解控制肿瘤转移至肝脏等远处器官部位过程的遗传因素,可能是提高结肠癌患者生存率的关键。通过将标准细胞遗传学技术与比较基因组杂交相结合,在先前根据肝转移行为差异选择的三个人类结肠癌细胞系中,鉴定出了多个遗传失衡情况。将一个低转移细胞系(KM12C)的整个基因组与从中衍生出的两个高转移细胞系(KM12SM、KM12L4A)的基因组直接进行比较。三个细胞系均存在一些常见的染色体增加(8q、12q15、20q11.2)和缺失(5p13、6p21.3、18),这些可能与肿瘤早期发展有关,而非与用于生成具有更高转移潜能细胞系的选择过程相关。在高转移细胞系中仅检测到的染色体失衡情况也被观察到。KM12SM显示2p22、2q24.3→2q32.2、4p15.3→cen、4q24部分缺失,且没有KM12C中所观察到的13q和15q22.3增加。KM12L4A既存在增加(1p31.3→1p21、2q22→2q33、3cen→3q26.2、5q14→5q23、6cen→6q23)也存在缺失(16p、17p、17q、19p、19q、22q),而其他两个细胞系未出现这些情况。这些改变的鉴定为实验性肝转移过程提供了有价值的见解,是朝着绘制与人类结肠癌进展终末期相关基因迈出的第一步。

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