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Autoantibody Profiling of Glioma Serum Samples to Identify Biomarkers Using Human Proteome Arrays

机译:胶质瘤血清样品的自身抗体分析,以鉴定使用人蛋白质组阵列的生物标志物

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The heterogeneity and poor prognosis associated with gliomas, makes biomarker identification imperative. Here, we report autoantibody signatures across various grades of glioma serum samples and sub-categories of glioblastoma multiforme using Human Proteome chips containing ~17000 full-length human proteins. The deduced sets of classifier proteins helped to distinguish Grade II, III and IV samples from the healthy subjects with 88, 89 and 94% sensitivity and 87, 100 and 73% specificity, respectively. Proteins namely, SNX1, EYA1, PQBP1 and IGHG1 showed dysregulation across various grades. Sub-classes of GBM, based on its proximity to the sub-ventricular zone, have been reported to have different prognostic outcomes. To this end, we identified dysregulation of NEDD9, a protein involved in cell migration, with probable prognostic potential. Another subcategory of patients where the IDH1 gene is mutated, are known to have better prognosis as compared to patients carrying the wild type gene. On a comparison of these two cohorts, we found STUB1 and YWHAH proteins dysregulated in Grade II glioma patients. In addition to common pathways associated with tumourigenesis, we found enrichment of immunoregulatory and cytoskeletal remodelling pathways, emphasizing the need to explore biochemical alterations arising due to autoimmune responses in glioma.
机译:与胶质瘤相关的异质性和不良预后,使得生物标志物鉴定势在必行。在这里,我们通过含有〜17000个全长人蛋白的人蛋白质组芯片报告各种胶质瘤血清样本和胶质母细胞瘤的胶质母细胞瘤血清样本和子类别的自身抗体型签名。推导的分类器蛋白组有助于将II级,III和IV样品与88,89和94%的敏感性分别区分,分别与87%和94%的敏感性和87,100和73%的特异性区分。蛋白质即,SNX1,EyA1,PQBP1和IGGG1在各种等级上显示了困难。据报道,GBM的亚类GBM的阶类已经据报道,具有不同的预后结果。为此,我们确定了NEDD9的失调,一种参与细胞迁移的蛋白质,具有可能的预后潜力。与携带野生型基因的患者相比,已知突变IDH1基因的患者的另一个患者子类别。在这两个队列的比较上,我们发现在II级胶质瘤患者中的短缺1和Ywhah蛋白。除了与肿瘤术相关的常见途径外,我们还发现富集免疫调节和细胞骨骼改造途径,强调需要探讨由于胶质瘤的自身免疫反应引起的生化改变。

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