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The Δ133p53β isoform promotes an immunosuppressive environment leading to aggressive prostate cancer

机译:Δ133p53β同种型促进免疫抑制环境,导致侵略性前列腺癌

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摘要

Prostate cancer is the second most common cancer in men, for which there are no reliable biomarkers or targeted therapies. Here we demonstrate that elevated levels of Δ133TP53β isoform characterize prostate cancers with immune cell infiltration, particularly T cells and CD163+ macrophages. These cancers are associated with shorter progression-free survival, Gleason scores?≥?7, and an immunosuppressive environment defined by a higher proportion of PD-1, PD-L1 and colony-stimulating factor 1 receptor (CSF1R) positive cells. Consistent with this, RNA-seq of tumours showed enrichment for pathways associated with immune signalling and cell migration. We further show a role for hypoxia and wild-type p53 in upregulating Δ133TP53 levels. Finally, AUC analysis showed that Δ133TP53β expression level alone predicted aggressive disease with 88% accuracy. Our data identify Δ133TP53β as a highly accurate prognostic factor for aggressive prostate cancer.
机译:前列腺癌是男性中最常见的癌症,没有可靠的生物标志物或有针对性的疗法。在这里,我们证明Δ1337TP53β同种型的升高,表征具有免疫细胞浸润的前列腺癌,特别是T细胞和CD163 +巨噬细胞。这些癌症与无进展的存活率较短,glason得分Δ≥17,以及由较高比例的PD-1,PD-L1和菌落刺激因子1受体(CSF1R)阳性细胞定义的免疫抑制环境。符合此,肿瘤的RNA-SEQ显示出与免疫信号传导和细胞迁移相关的途径的富集。我们进一步表明缺氧和野生型P53在上调Δ1337TP53水平中的作用。最后,AUC分析表明,δ133TP53β表达水平单独预测伴随症状,精度为88%。我们的数据鉴定Δ1337TP53β作为侵袭性前列腺癌的高度准确的预后因素。

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