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印刷肽阵列可识别胶质母细胞瘤患者的预后性腱生蛋白C血清抗体。

Printed peptide arrays identify prognostic TNC serumantibodies in glioblastoma patients.

作者信息

Mock Andreas, Warta Rolf, Geisenberger Christoph, Bischoff Ralf, Schulte Alexander, Lamszus Katrin, Stadler Volker, Felgenhauer Thomas, Schichor Christian, Schwartz Christoph, Matschke Jakob, Jungk Christine, Ahmadi Rezvan, Sahm Felix, Capper David, Glass Rainer, Tonn Jörg-Christian, Westphal Manfred, von Deimling Andreas, Unterberg Andreas, Bermejo Justo Lorenzo, Herold-Mende Christel

机构信息

Department of Neurosurgery, Experimental Neurosurgery, University of Heidelberg, Heidelberg, Germany.

PEPperPRINT GmbH, Heidelberg, Germany.

出版信息

Oncotarget. 2015 May 30;6(15):13579-90. doi: 10.18632/oncotarget.3791.

Abstract

Liquid biopsies come of age offering unexploited potential to monitor and react to tumor evolution. We developed a cost-effective assay to non-invasively determine the immune status of glioblastoma (GBM) patients. Employing newly developed printed peptide microarrays we assessed the B-cell response against tumor-associated antigens (TAAs) in 214 patients. Firstly, sera of long-term (36+ months, LTS, n=10) and short-term (6-10 months, STS, n=14) surviving patients were screened for prognostic antibodies against 1745 13-mer peptides covering known TAAs (TNC, EGFR, GLEA2, PHF3, FABP5, MAGEA3). Next, survival associations were investigated in two retrospective independent multicenter validation sets (n=61, n=129, all IDH1-wildtype). Reliability of measurements was tested using a second array technology (spotted arrays). LTS/STS screening analyses identified 106 differential antibody responses. Evaluating the Top30 peptides in validation set 1 revealed three prognostic peptides. Prediction of TNC peptide VCEDGFTGPDCAE was confirmed in a second set (p=0.043, HR=0.66 [0.44-0.99]) and was unrelated to TNC protein expression. Median signals of printed arrays correlated with pre-synthesized spotted microarrays (p<0.0002, R=0.33). Multiple survival analysis revealed independence of age, gender, KPI and MGMT status. We present a novel peptide microarray immune assay that identified increased anti-TNC VCEDGFTGPDCAE serum antibody titer as a promising non-invasive biomarker for prolonged survival.

摘要

液体活检已步入成熟阶段,为监测肿瘤演变并做出反应提供了尚未开发的潜力。我们开发了一种经济高效的检测方法,用于非侵入性地确定胶质母细胞瘤(GBM)患者的免疫状态。利用新开发的打印肽微阵列,我们评估了214例患者针对肿瘤相关抗原(TAA)的B细胞反应。首先,对长期存活(36个月以上,LTS,n = 10)和短期存活(6 - 10个月,STS,n = 14)患者的血清进行筛查,以寻找针对1745种覆盖已知TAA(TNC、EGFR、GLEA2、PHF3、FABP5、MAGEA3)的13肽的预后抗体。接下来,在两个回顾性独立多中心验证组(n = 61,n = 129,均为IDH1野生型)中研究生存相关性。使用第二种阵列技术(点阵式阵列)测试测量的可靠性。LTS/STS筛查分析确定了106种差异抗体反应。在验证组1中评估前30种肽,发现了三种预后肽。在第二组中证实了TNC肽VCEDGFTGPDCAE的预测(p = 0.043,HR = 0.66 [0.44 - 0.99]),且与TNC蛋白表达无关。打印阵列的中位信号与预合成的点阵式微阵列相关(p < 0.0002,R = 0.33)。多因素生存分析显示年龄、性别、关键性能指标和MGMT状态具有独立性。我们提出了一种新型肽微阵列免疫检测方法,该方法确定抗TNC VCEDGFTGPDCAE血清抗体滴度升高是延长生存期的一种有前景的非侵入性生物标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/50c1/4537035/01e9ad33d250/oncotarget-06-13579-g001.jpg

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