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Clinical and prognostic implications of an immune‐related risk model based on TP53 status in lung adenocarcinoma
Authors:Xuming Song  Qiang Chen  Jifan Wang  Qixing Mao  Wenjie Xia  Lin Xu  Feng Jiang  Gaochao Dong
Institution:1. The Affiliated Cancer Hospital of Nanjing Medical University, Nanjing China ; 2. Department of Thoracic Surgery, Jiangsu Cancer Hospital, Jiangsu Institute of Cancer Research, Nanjing China ; 3. Jiangsu Key Laboratory of Molecular and Translational Cancer Research, Cancer Institute of Jiangsu Province, Nanjing China ; 4. The Fourth Clinical College of Nanjing Medical University, Nanjing China ; 5. XuZhou Central Hospital, Xuzhou China
Abstract:TP53 mutation is the most widespread mutation in lung adenocarcinoma (LUAD). Meanwhile, p53 (encoded by TP53) has recently been implicated in immune responses. However, it is still unknown whether TP53 mutation remodels the tumour microenvironment to influence tumour progression and prognosis in LUAD. In this study, we developed a 6‐gene immune‐related risk model (IRM) to predict the survival of patients with LUAD in The Cancer Genome Atlas (TCGA) cohort based on TP53 status, and the predictive ability was confirmed in 2 independent cohorts. TP53 mutation led to a decreased immune response in LUAD. Further analysis revealed that patients in the high‐index group had observably lower relative infiltration of memory B cells and regulatory T cells and significantly higher relative infiltration of neutrophils and resting memory CD4+ T cells. Additionally, the IRM index positively correlated with the expression of critical immune checkpoint genes, including PDCD1 (encoding PD‐1) and CD274 (encoding PD‐L1), which was validated in the Nanjing cohort. Furthermore, as an independent prognostic factor, the IRM index was used to establish a nomogram for clinical application. In conclusion, this IRM may serve as a powerful prognostic tool to further optimize LUAD immunotherapy.
Keywords:immune profile  immune prognostic model  lung adenocarcinoma  TP53   mutation
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