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首页> 外文期刊>CNS neuroscience & therapeutics. >Costimulatory checkpoint SLAMF8 is an independent prognosis factor in glioma
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Costimulatory checkpoint SLAMF8 is an independent prognosis factor in glioma

机译:共刺激检查点SLAMF8是神经胶质瘤的独立预后因素

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Aims Immune checkpoint blockade has made breakthroughs in immunotherapy for glioma. However, current immunotherapy has therapeutic benefits only in a subset of patients and accompanied by immune‐related side effects. SLAMF8 is a costimulatory molecule that affects the activation of macrophages in inflammation. The study of SLAMF8 may provide new information for immunological research and treatment of glioma. Methods CGGA and TCGA cohorts of 946 patients with RNA sequencing data and full clinical information were analyzed using R language and GraphPad Prism 7. Results SLAMF8 was overexpressed along with malignancy progression and was a biomarker of mesenchymal subtype. As an independent prognostic factor, high SLAMF8 conferred reduced overall survival and chemotherapy resistance. SLAMF8 implied lower proportion of cancer cells along with increasing enrichment of monocytic lineage, myeloid dendritic cells. Functional analysis showed higher SLAMF8 indicated activation of antigen processing and presenting and the IFN‐γ/TNF/TLR‐mediated signaling. Meanwhile, coexpressing with classical checkpoint SLAMF8 aggravated immunosuppression and enhanced inflammation response. Conclusion Our study highlighted the important role of SLAMF8 in malignancy progression, shortened survival, and immune disorders. Further research on SLAMF8 in immunosuppression and inflammation response to glioma cells could aid immunotherapy for glioma.
机译:目的免疫检查点封锁在神经胶质瘤免疫治疗方面取得了突破。但是,当前的免疫疗法仅在部分患者中具有治疗益处,并伴有免疫相关的副作用。 SLAMF8是一种共刺激分子,可影响炎症反应中巨噬细胞的活化。 SLAMF8的研究可能为神经胶质瘤的免疫学研究和治疗提供新的信息。方法使用R语言和GraphPad Prism 7对946例具有RNA测序数据和完整临床信息的患者的CGGA和TCGA队列进行分析。结果SLAMF8过度表达,伴随恶性进展,是间充质亚型的生物标志物。作为独立的预后因素,高SLAMF8会降低总生存期和化疗耐药性。 SLAMF8暗示癌细胞的比例降低,同时单核细胞系,髓样树突状细胞的富集度增加。功能分析表明,较高的SLAMF8表示激活了抗原加工和呈递以及IFN-γ/ TNF / TLR介导的信号传导。同时,与经典检查点SLAMF8共表达可加重免疫抑制并增强炎症反应。结论我们的研究强调了SLAMF8在恶性肿瘤进展,缩短生存期和免疫疾病中的重要作用。 SLAMF8在神经胶质瘤细胞的免疫抑制和炎症反应中的进一步研究可能有助于神经胶质瘤的免疫治疗。

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