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酪氨酸激酶基因ACK1的转移特性与基因组扩增

Metastatic properties and genomic amplification of the tyrosine kinase gene ACK1.

作者信息

van der Horst Edward Htun, Degenhardt Yan Y, Strelow Astrid, Slavin Anthony, Chinn Lawrence, Orf Jessica, Rong Minqing, Li Shyun, See Lei-Hoon, Nguyen Ken Q C, Hoey Timothy, Wesche Holger, Powers Scott

机构信息

Department of Biology, Amgen, Inc., 1120 Veterans Boulevard, South San Francisco, CA 94080, USA.

出版信息

Proc Natl Acad Sci U S A. 2005 Nov 1;102(44):15901-6. doi: 10.1073/pnas.0508014102. Epub 2005 Oct 24.

Abstract

Metastasis of primary tumors leads to a very poor prognosis for patients suffering from cancer. Although it is well established that not every tumor will eventually metastasize, it is less clear whether primary tumors acquire genetic alterations in a stochastic process at a late stage, which make them invasive, or whether genetic alterations acquired early in the process of tumor development drive primary tumor growth and determine whether this tumor is going to be metastatic. To address this issue, we tested genes identified in a large-scale comparative genomic hybridization analysis of primary tumor for their ability to confer metastatic properties on a cancer cell. We identified amplification of the ACK1 gene in primary tumors, which correlates with poor prognosis. We further show that overexpression of Ack1 in cancer cell lines can increase the invasive phenotype of these cells both in vitro and in vivo and leads to increased mortality in a mouse model of metastasis. Biochemical studies show that Ack1 is involved in extracellular matrix-induced integrin signaling, ultimately activating signaling processes like the activation of the small GTPase Rac. Taken together, this study supports a theory from Bernards and Weinberg [Bernards, R. & Weinberg, R. A. (2002) Nature 418, 823], which postulates that the tendency to metastasize is largely predetermined.

摘要

原发性肿瘤的转移会导致癌症患者的预后非常差。虽然大家都清楚并非每个肿瘤最终都会发生转移,但尚不清楚原发性肿瘤是在晚期通过随机过程获得使它们具有侵袭性的基因改变,还是在肿瘤发展过程早期获得的基因改变驱动原发性肿瘤生长并决定该肿瘤是否会发生转移。为了解决这个问题,我们测试了在原发性肿瘤的大规模比较基因组杂交分析中鉴定出的基因赋予癌细胞转移特性的能力。我们发现原发性肿瘤中ACK1基因的扩增与预后不良相关。我们进一步表明,在癌细胞系中过表达Ack1可在体外和体内增加这些细胞的侵袭表型,并导致转移小鼠模型中的死亡率增加。生化研究表明,Ack1参与细胞外基质诱导的整合素信号传导,最终激活诸如小GTP酶Rac激活等信号传导过程。综上所述,本研究支持Bernards和Weinberg提出的理论[Bernards, R. & Weinberg, R. A. (2002) Nature 418, 823],该理论假设转移倾向在很大程度上是预先确定的。

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