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肿瘤内坏死相关细胞因子模式的表达与胶质瘤的预后和免疫状态相关。

Expression of intra-tumoral necrosis-associated cytokine pattern correlated with prognosis and immune status in glioma.

作者信息

Zhao Hongtao, Dong Jiawei, Zhang Jiheng, Wang Nan, Liu Zhihui, Yan Xiuwei, Wang Fang, Ji Hang, Hu Shaoshan

机构信息

Cancer Center, Department of Neurosurgery, Zhejiang Provincial People's Hospital, Affiliated People's Hospital, Hangzhou Medical College, Hangzhou, Zhejiang, China.

Department of Neurosurgery, West China Hospital, Sichuan University, Chengdu, China.

出版信息

Front Mol Neurosci. 2023 Jul 3;16:1117237. doi: 10.3389/fnmol.2023.1117237. eCollection 2023.

Abstract

Intra-tumoral necrosis (ITN) is reported to be an independent prognostic factor in glioma. However, knowledge of ITN is mainly limited to pseudopalisadwe, while its other aspects were neglected. Therefore, a deeper understanding of ITN could be valuable for understanding its exact role in glioma. The only reliable ITN model was time-dependently achieved with the GL261 syngeneic mouse model. The ITN-associated expression pattern was enriched from RNA sequencing. TCGA glioma samples were clustered into a high-expression group (HEG) and a low-expression group (LEG) based on their pattern and their association with prognosis, clinical status, immune status, and therapeutic responsiveness were compared. Mouse glioma with ITN demonstrated invasive histology. Cytokine signaling was significantly enriched in necrotic mouse glioma compared with non-necrotic glioma tissues. Nine pro-inflammatory (IL6, PPBP, IL1A, TNFSF11, CXCL11, CXCL9, CXCL10, CXCL3, and CCL8) and two anti-inflammatory cytokine (IL1RN and IL10) genes were found to be related to ITN-associated cytokine patterns. Comparative analysis showed that HEG had a significantly shorter survival time, five differentially distributed clinical statuses, more infiltrated immune cells, greater expression of immune checkpoints, and better therapeutic responsiveness than LEG. In conclusion, the ITN-associated cytokine pattern is characteristically expressed in glioma with ITN and might indicate necrosis missed in histology diagnosis. Its expression pattern could predict the prognosis, tumor grade, immune status, and therapeutic responsiveness of glioma patients.

摘要

肿瘤内坏死(ITN)据报道是胶质瘤的一个独立预后因素。然而,对ITN的了解主要局限于假栅栏状坏死,而其其他方面则被忽视。因此,更深入地了解ITN对于理解其在胶质瘤中的确切作用可能具有重要价值。通过GL261同基因小鼠模型随时间依赖性地建立了唯一可靠的ITN模型。从RNA测序中富集了与ITN相关的表达模式。根据TCGA胶质瘤样本的模式将其聚类为高表达组(HEG)和低表达组(LEG),并比较了它们与预后、临床状态、免疫状态和治疗反应性的关联。具有ITN的小鼠胶质瘤表现出侵袭性组织学特征。与非坏死性胶质瘤组织相比,坏死性小鼠胶质瘤中细胞因子信号通路显著富集。发现9种促炎细胞因子(IL6、PPBP、IL1A、TNFSF11、CXCL11、CXCL9、CXCL10、CXCL3和CCL8)和2种抗炎细胞因子(IL1RN和IL10)基因与ITN相关的细胞因子模式有关。比较分析表明,与LEG相比,HEG的生存时间明显更短,有5种不同分布的临床状态,免疫细胞浸润更多,免疫检查点的表达更高,治疗反应性更好。总之,与ITN相关的细胞因子模式在伴有ITN的胶质瘤中具有特征性表达,可能提示组织学诊断中遗漏的坏死。其表达模式可以预测胶质瘤患者的预后、肿瘤分级、免疫状态和治疗反应性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7e9d/10352027/a0fcb9a0e91b/fnmol-16-1117237-g001.jpg

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