McIntyre Alan, Summersgill Brenda, Spendlove Hayley E, Huddart Robert, Houlston Richard, Shipley Janet
Molecular Cytogenetics, Section of Molecular Carcinogenesis, The Institute of Cancer Research, Sutton, Surrey, UK.
Neoplasia. 2005 Dec;7(12):1047-52. doi: 10.1593/neo.05514.
Amplification and/or overexpression of genes encoding tyrosine kinase receptors KIT and ERBB2 have been reported in testicular germ cell tumors (TGCTs). These receptors can bind the adaptor molecule GRB7 encoded by a gene adjacent to ERBB2 at 17q12, a region also frequently gained in TGCTs. GRB7 binding may be involved in the activation of RAS signaling and KRAS2 maps to 12p, which is constitutively gained in TGCT and lies within a minimum overlapping region of amplification at 12p11.2-12.1, a region we have previously defined. RAS proteins activate BRAF, and activating mutations of genes encoding these proteins have been described in various tumors. Here we determine the relationships between expression levels and activating mutations of these genes in a series of 65 primary TGCTs and 4 TCGT cell lines. High levels of expression and activating mutations in RAS were mutually exclusive events, and activating mutations in RAS were only identified in the seminoma subtype. Mutations in BRAF were not identified. Increased ERBB2 expression was associated with differentiated nonseminoma histology excised from lymph nodes postchemotherapy. Mutation, elevated expression, and correlations between expression levels of KRAS2, GRB7, and KIT are consistent with their involvement in the development of TGCTs.
在睾丸生殖细胞肿瘤(TGCTs)中,已报道编码酪氨酸激酶受体KIT和ERBB2的基因存在扩增和/或过表达。这些受体可结合由位于17q12的与ERBB2相邻的基因编码的衔接分子GRB7,该区域在TGCTs中也经常扩增。GRB7的结合可能参与RAS信号通路的激活,而KRAS2定位于12p,在TGCT中该区域呈组成性扩增,位于我们之前定义的12p11.2 - 12.1最小重叠扩增区域内。RAS蛋白激活BRAF,并且在各种肿瘤中已描述了编码这些蛋白的基因的激活突变。在此,我们确定了在一系列65例原发性TGCT和4个TCGT细胞系中这些基因的表达水平与激活突变之间的关系。RAS中的高水平表达和激活突变是相互排斥的事件,并且RAS中的激活突变仅在精原细胞瘤亚型中被鉴定到。未鉴定到BRAF的突变。ERBB2表达增加与化疗后从淋巴结切除的分化型非精原细胞瘤组织学相关。KRAS2、GRB7和KIT的突变、表达升高以及表达水平之间的相关性与其在TGCTs发生中的作用一致。
