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Expression array analysis of the hepatocyte growth factor invasive program

机译:肝细胞生长因子侵袭性程序的表达阵列分析

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Signaling by human hepatocyte growth factor (hHGF) via its cell surface receptor (MET) drives mitogenesis, motogenesis and morphogenesis in a wide spectrum of target cell types and embryologic, developmental and homeostatic contexts. Oncogenic pathway activation also contributes to tumorigenesis and cancer progression, including tumor angiogenesis and metastasis, in several prevalent malignancies. The HGF gene encodes full-length hHGF and two truncated isoforms known as NK1 and NK2. NK1 induces all three HGF activities at modestly reduced potency, whereas NK2 stimulates only motogenesis and enhances HGF-driven tumor metastasis in transgenic mice. Prior studies have shown that mouse HGF (mHGF) also binds with high affinity to human MET. Here we show that, like NK2, mHGF stimulates cell motility, invasion and spontaneous metastasis of PC3M human prostate adenocarcinoma cells in mice through human MET. To identify target genes and signaling pathways associated with motogenic and metastatic HGF signaling, i.e., the HGF invasive program, gene expression profiling was performed using PC3M cells treated with hHGF, NK2 or mHGF. Results obtained using Ingenuity Pathway Analysis software showed significant overlap with networks and pathways involved in cell movement and metastasis. Interrogating The Cancer Genome Atlas project also identified a subset of 23 gene expression changes in PC3M with a strong tendency for co-occurrence in prostate cancer patients that were associated with significantly decreased disease-free survival.
机译:人肝细胞生长因子(hHGF)通过其细胞表面受体(MET)发出的信号在广泛的靶细胞类型以及胚胎学,发育和体内平衡环境中驱动有丝分裂,动生和形态发生。致癌途径激活还促进了几种流行的恶性肿瘤的肿瘤发生和癌症进展,包括肿瘤血管生成和转移。 HGF基因编码全长hHGF和两个截短的亚型,称为NK1和NK2。 NK1在适度降低的效力下诱导所有三种HGF活性,而NK2仅刺激转基因小鼠的运动发生并增强HGF驱动的肿瘤转移。先前的研究表明,小鼠HGF(mHGF)也与人MET具有很高的亲和力。在这里,我们显示,与NK2一样,mHGF通过人MET刺激小鼠PC3M人前列腺腺癌细胞的细胞运动,侵袭和自发转移。为了鉴定与运动原性和转移性HGF信号转导相关的靶基因和信号通路,即HGF侵入性程序,使用经hHGF,NK2或mHGF处理的PC3M细胞进行基因表达谱分析。使用Ingenuity Pathway Analysis软件获得的结果显示与细胞移动和转移所涉及的网络和途径有明显的重叠。审讯癌症基因组图谱项目还确定了PC3M中23个基因表达变化的一个子集,在前列腺癌患者中有很强的共现趋势,这与无病生存期明显减少有关。

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