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鉴定和功能表征肾细胞癌中 pVHL 依赖性细胞表面蛋白。

Identification and functional characterization of pVHL-dependent cell surface proteins in renal cell carcinoma.

机构信息

Institute of Surgical Pathology, University Hospital Zurich, Zurich, Switzerland.

出版信息

Neoplasia. 2012 Jun;14(6):535-46. doi: 10.1596/neo.12130.

Abstract

The identification of cell surface accessible biomarkers enabling diagnosis, disease monitoring, and treatment of renal cell carcinoma (RCC) is as challenging as the biology and progression of RCC is unpredictable. A hallmark of most RCC is the loss-of-function of the von Hippel-Lindau (pVHL) protein by mutation of its gene (VHL). Using the cell surface capturing (CSC) technology, we screened and identified cell surface N-glycoproteins in pVHL-negative and positive 786-O cells. One hundred six cell surface N-glycoproteins were identified. Stable isotope labeling with amino acids in cell culture-based quantification of the CSC screen revealed 23 N-glycoproteins whose abundance seemed to change in a pVHL-dependent manner. Targeted validation experiments using transcriptional profiling of primary RCC samples revealed that nine glycoproteins, including CD10 and AXL, could be directly linked to pVHL-mediated transcriptional regulation. Subsequent human tumor tissue analysis of these cell surface candidate markers showed a correlation between epithelial AXL expression and aggressive tumor phenotype, indicating that pVHL-dependent regulation of glycoproteins may influence the biologic behavior of RCC. Functional characterization of the metalloprotease CD10 in cell invasion assays demonstrated a diminished penetrating behavior of pVHL-negative 786-O cells on treatment with the CD10-specific inhibitor thiorphan. Our proteomic surfaceome screening approach in combination with transcriptional profiling and functional validation suggests pVHL-dependent cell surface glycoproteins as potential diagnostic markers for therapeutic targeting and RCC patient monitoring.

摘要

鉴定能够用于诊断、疾病监测和治疗肾细胞癌(RCC)的细胞表面可及生物标志物,与 RCC 的生物学和进展一样具有挑战性,因为 RCC 的进展是不可预测的。大多数 RCC 的一个标志是其基因(VHL)发生突变导致von Hippel-Lindau(pVHL)蛋白功能丧失。我们使用细胞表面捕获(CSC)技术筛选和鉴定了 pVHL 阴性和阳性 786-O 细胞中的细胞表面 N-糖蛋白。鉴定出 106 种细胞表面 N-糖蛋白。基于细胞培养的稳定同位素标记与氨基酸定量的 CSC 筛选显示,23 种 N-糖蛋白的丰度似乎以 pVHL 依赖的方式发生变化。使用原发性 RCC 样本的转录谱进行的靶向验证实验表明,包括 CD10 和 AXL 在内的 9 种糖蛋白可以直接与 pVHL 介导的转录调控相关联。对这些细胞表面候选标志物的人类肿瘤组织分析表明,上皮细胞 AXL 表达与侵袭性肿瘤表型之间存在相关性,表明糖蛋白的 pVHL 依赖性调节可能影响 RCC 的生物学行为。在细胞侵袭实验中对金属蛋白酶 CD10 的功能特征进行了表征,结果表明,pVHL 阴性的 786-O 细胞在用 CD10 特异性抑制剂硫醇肽处理后,穿透行为减弱。我们的蛋白质组学表面组筛选方法结合转录谱分析和功能验证表明,pVHL 依赖性细胞表面糖蛋白可能是治疗靶点和 RCC 患者监测的潜在诊断标志物。

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