睾丸癌抗原DDX53作为潜在的早期食管癌抗原的免疫信息学评估。

Oncoscience Pub Date : 2023-11-10 eCollection Date: 2023-01-01 DOI:10.18632/oncoscience.590
Peter Cheng, Konrad J Cios, Mallika Varkhedi, Vayda R Barker, Michelle Yeagley, Andrea Chobrutskiy, Boris I Chobrutskiy, George Blanck
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引用次数: 0

摘要

t淋巴细胞参与促进促炎、促肿瘤微环境,从而恶化食管癌(ESCA)的预后。在本研究中,我们鉴定了肿瘤驻留t细胞受体(TCR)互补决定区3 (CDR3)氨基酸序列,并采用特别适合大数据设置的算法来评估TCR CDR3-癌睾丸抗原(CTA)化学互补。ESCA TCR CDR3s和睾丸癌抗原DDX53的化学互补性代表了无病生存(DFS)的区别,其中,50百分位互补性较高的组与较差的DFS相关。高TCR CDR3-DDX53互补组也代表了更大比例的缺乏DDX53表达的肿瘤样本。这些数据和分析提出了一个问题,即TCR CDR3-DDX53化学互补性评估是否检测到选择ddx53阴性细胞的ESCA免疫反应?
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An immunoinformatics assessment of the cancer testis antigen, DDX53, as a potential early esophageal cancer antigen.

T-lymphocytes have been implicated in facilitating a pro-inflammatory, pro-tumorigenic microenvironment that worsens prognosis for esophageal carcinoma (ESCA). In this study, we identified tumor resident, T-cell receptor (TCR) complementarity determining region-3 (CDR3) amino acid sequences and employed an algorithm particularly suited to the big data setting to evaluate TCR CDR3-cancer testis antigen (CTA) chemical complementarities. Chemical complementarity of the ESCA TCR CDR3s and the cancer testis antigen DDX53 represented a disease-free survival (DFS) distinction, whereby the upper fiftieth percentile complementarity group correlated with worse DFS. The high TCR CDR3-DDX53 complementarity group also represented a greater proportion of tumor samples lacking DDX53 expression. These data and analyses raise the question of whether the TCR CDR3-DDX53 chemical complementarity assessment detected an ESCA immune response that selected for DDX53-negative cells?

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