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FGF 受体 4 多态性等位基因对结肠癌生长和转移的影响差异。

Differential effects of polymorphic alleles of FGF receptor 4 on colon cancer growth and metastasis.

机构信息

Department of Medicine 1, Institute of Cancer Research, Clinical Institute of Pathology, University of Vienna, Vienna, Austria.

出版信息

Cancer Res. 2012 Nov 15;72(22):5767-77. doi: 10.1158/0008-5472.CAN-11-3654. Epub 2012 Sep 12.

DOI:10.1158/0008-5472.CAN-11-3654
PMID:22971346
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5455878/
Abstract

A gly(388)arg polymorphism (rs351855) in the transmembrane domain of the fibroblast growth factor receptor (FGFR4) is associated with increased risk, staging, and metastasis in several different types of cancer. To specifically assess the impact of the polymorphic FGFR4 in colorectal cancer (CRC), we engineered CRC cell lines with distinct endogenous expression patterns to overexpress either the FGFR4(gly) or FGFR4(arg) alleles. The biologic analyses revealed an oncogenic importance for both polymorphic alleles, but FGFR4(gly) was the stronger inducer of tumor growth, whereas FGFR4(arg) was the stronger inducer of migration. An evaluation of clinical specimens revealed that FGFR4 was upregulated in 20/71 patients independent of gly(388)arg status. There was no correlation between the presence of an FGFR4(arg) allele and CRC or polyp risk in 3,471 participants of the CORSA study. However, among 182 patients with CRC, FGFR4(arg)-carriers had a fivefold higher risk of tumors that were stage II or greater. Together, our results established that both allelic forms of FGFR4 exert an oncogenic impact and may serve equally well as therapeutic targets in CRC. One important implication of our findings is that FGFR4(arg)-carriers are at a higher risk for more aggressive tumors and therefore may profit from early detection measures.

摘要

成纤维细胞生长因子受体(FGFR4)跨膜结构域中的一个 gly(388)arg 多态性(rs351855)与多种不同类型癌症的风险增加、分期和转移有关。为了专门评估多态性 FGFR4 在结直肠癌(CRC)中的影响,我们设计了具有不同内源性表达模式的 CRC 细胞系,以过表达 FGFR4(gly)或 FGFR4(arg)等位基因。生物学分析表明,这两种多态等位基因都具有致癌作用,但 FGFR4(gly)是更强的肿瘤生长诱导剂,而 FGFR4(arg)是更强的迁移诱导剂。对临床标本的评估表明,FGFR4 在 20/71 例患者中上调,与 gly(388)arg 状态无关。在 CORSA 研究的 3471 名参与者中,FGFR4(arg)等位基因的存在与 CRC 或息肉风险之间没有相关性。然而,在 182 名 CRC 患者中,FGFR4(arg)携带者 II 期或更高级别肿瘤的风险增加了五倍。总之,我们的研究结果表明,FGFR4 的两种等位基因形式都具有致癌作用,并且可以作为 CRC 的治疗靶点。我们研究结果的一个重要意义是,FGFR4(arg)携带者更容易发生侵袭性肿瘤,因此可能受益于早期检测措施。

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