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细胞系 secretome,一种用于研究肿瘤体内释放的蛋白质的合适工具:应用于肺癌细胞中 p53 调节的蛋白质分泌的研究。

The cell line secretome, a suitable tool for investigating proteins released in vivo by tumors: application to the study of p53-modulated proteins secreted in lung cancer cells.

机构信息

Université Joseph Fourier-Grenoble 1, INSERM, Institut Albert Bonniot U823, Grenoble, France.

出版信息

J Proteome Res. 2009 Oct;8(10):4579-91. doi: 10.1021/pr900383g.

DOI:10.1021/pr900383g
PMID:19639960
Abstract

Malignant processes such as metastasis, invasion, or angiogenesis are tightly dependent on the composition of the extracellular medium, which is itself affected by the release of proteins by the tumor cells. p53, a major tumor suppressor protein very frequently mutated and/or inactivated in cancer cells, is known to modulate the release of proteins by the tumor cells; however, while p53-modulated intracellular proteins have been extensively studied, little is known concerning their extracellular counterparts. Here, we characterized the p53-dependent secretome of a lung tumor model in vitro (H358 human nonsmall cell lung adenocarcinoma cell line with a homozygous deletion of p53) and demonstrate that the modulation of exported proteins can also be detected in vivo in the plasma of tumor-bearing mice. We used a clone of H358, stably transfected with a tetracycline-inducible wild-type p53-expressing vector. With the use of iTRAQ labeling and LC-MALDI-MS/MS analysis, we identified 909 proteins released in vitro by the cells, among which 91 are p53-modulated. Three proteins (GDF-15, FGF-19, and VEGF) were also investigated in H358/TetOn/p53 xenograft mice. The ELISA dosage on total tumor protein extracts confirmed the influence of p53 on the release of these proteins in vivo. Moreover, the GDF-15 concentration was measured in the plasma and its p53-dependent modulation was confirmed. To our knowledge, this is the first report establishing that the in vitro cell line secretome is reliable and reflects the extracellular release of proteins from tumor cells in vivo and could be used to identify putative tumor markers.

摘要

恶性过程,如转移、侵袭或血管生成,与细胞外基质的组成密切相关,而细胞外基质本身也受到肿瘤细胞释放的蛋白质的影响。p53 是一种主要的肿瘤抑制蛋白,在癌细胞中经常发生突变和/或失活,已知它可以调节肿瘤细胞释放蛋白质;然而,尽管已经对 p53 调节的细胞内蛋白质进行了广泛的研究,但对于其细胞外对应物知之甚少。在这里,我们在体外(H358 人非小细胞肺癌腺癌细胞系,p53 纯合缺失)肺肿瘤模型中表征了 p53 依赖性分泌组,并证明了在荷瘤小鼠的血浆中也可以检测到对输出蛋白的调节。我们使用了一种 H358 的克隆,它稳定转染了一种四环素诱导的野生型 p53 表达载体。使用 iTRAQ 标记和 LC-MALDI-MS/MS 分析,我们鉴定了细胞体外释放的 909 种蛋白质,其中 91 种受 p53 调节。还在 H358/TetOn/p53 异种移植小鼠中研究了三种蛋白质(GDF-15、FGF-19 和 VEGF)。总肿瘤蛋白提取物的 ELISA 剂量证实了 p53 对这些蛋白质在体内释放的影响。此外,还测量了血浆中的 GDF-15 浓度,并证实了其受 p53 调节。据我们所知,这是第一个建立体外细胞系分泌组可靠并反映体内肿瘤细胞细胞外释放蛋白质的报告,可用于鉴定潜在的肿瘤标志物。

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