Identification of novel autoantibodies in ascites of relapsed paclitaxel-resistant gastric cancer with peritoneal metastasis using immunome protein microarrays and proteomics

腹水 紫杉醇 自身抗体 蛋白质组学 医学 转移 波形蛋白 蛋白质微阵列 癌症 组织微阵列 抗体微阵列 癌症研究 病理 免疫学 微阵列 抗体 内科学 生物 免疫组织化学 基因表达 生物化学 基因
作者
Zhongyin Yang,Chao Yan,Wentao Liu,Wei Xu,Chen Li,Min Yan,Bingya Liu,Zhenggang Zhu
出处
期刊:Cancer Biomarkers [IOS Press]
卷期号:31 (4): 329-338 被引量:5
标识
DOI:10.3233/cbm-203142
摘要

Gastric cancer (GC) patients with peritoneal metastasis usually have extremely poor prognosis. Intraperitoneal infusion of paclitaxel (PTX) provides an effective treatment, but relapse and PTX-resistance are unavoidable disadvantages, and it is difficult to monitor the occurrence of PTX-resistance.The aim of this study was to explore novel autoantibodies in the ascites of individuals with relapsed PTX-resistant GC with peritoneal metastasis.Ascites samples were collected before PTX infusion and after the relapse in 3 GC patients. To determine the expression of significantly changed proteins, we performed autoantibody profiling with immunome protein microarrays and tandem mass tag (TMT) quantitative proteomics, and then, the overlapping proteins were selected.Thirty-eight autoantibodies that were differentially expressed between the ascites in the untreated group and relapsed PTX-resistant group were identified. For confirmation of the results, TMT quantitative proteomics was performed, and 842 dysregulated proteins were identified. Four proteins, TPM3, EFHD2, KRT19 and vimentin, overlapped between these two assays.Our results first revealed that TPM3, EFHD2, KRT19 and vimentin were novel autoantibodies in the ascites of relapsed PTX-resistant GC patients. These autoantibodies may be used as potential biomarkers to monitor the occurrence of PTX-resistance.
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