Abstract
Immune checkpoint inhibitors (ICIs) effectively treat lung adenocarcinoma (LUAD) with fewer side effects. However, for LUAD patients, the lack of predictive markers for ICIs makes their clinical benefits less than ideal. Despite reports suggesting that a TTN (titin) mutation plays an important role in immunotherapy of solid tumors and gastric cancer, the relationship between the TTN mutation and LUAD immunotherapy has not been determined. We collected a LUAD cohort with whole-exome sequencing (WES) and immunotherapy prognosis. The ICI cohort was used to explore the relationship between TTN mutation status and prognosis. Then, the Cancer Genome Atlas (TCGA)-LUAD and Chen-LUAD cohorts were downloaded from the cbioportal website. We also used CIBERSORT, gene-set enrichment analysis (GSEA), and single-sample GSEA (ssGSEA) to evaluate the proportion of immune cells and the degree of pathway activation in LUAD patients, respectively. DDR signaling pathways obtained from the Molecular Signatures Database (MSigDB), tumor mutation burden (TMB), and NAL were used to evaluate the immunogenicity of LUAD patients. In the ICI cohort, TTN-mutant (TTN-MT) had significantly longer overall survival (OS) than TTN-wildtype (TTN-WT) (P = 0.009). Univariate and multivariate COX models showed that TTN mutation status can independently predict immunotherapy prognosis. Notably, the results of tumor immune microenvironment (TIME) analysis showed that TTN-MT patients had inflammatory TIME, which showed enriched activated immune cells and higher immune scores. Immunogenicity analysis showed higher immunogenicity in TTN-MT patients, which indicated high levels of gene mutations in TMB, NAL, and DDR pathways. GSEA and ssGSEA results showed that TTN-MT was substantially enriched in chemokine secretion, inflammatory factor secretion, and antigen presentation. Some pathways related to immunosuppression and immune depletion were significantly downregulated. TTN-MT is associated with significantly prolonged OS in LUAD patients. Additionally, TTN-MT is related to high immunogenicity and inflammatory TIME, suggesting that TTN-MT may be a potential predictive marker for patients with LUAD to accept ICIs.
Highlights
At present, lung cancer tumor malignancy presents with the highest rates of morbidity and mortality, while lung adenocarcinoma (LUAD) is the main subclass of primary lung cancer [1]
TTN-MT Is Related to the Prognosis of LUAD Patients Receiving Immunotherapy
We found that other clinical characteristics and tumor mutation burden (TMB), a known factor related to the immunotherapy prognosis, were not related to the prognosis of LUAD patients
Summary
Lung cancer tumor malignancy presents with the highest rates of morbidity and mortality, while lung adenocarcinoma (LUAD) is the main subclass of primary lung cancer (about 85%) [1]. LUAD has a long incubation period, mild early symptoms, and a high degree of malignancy. LUAD patients progress to the advanced stage at the time of diagnosis and miss the chance for treatment [2]. With the development of various targeted drugs and their application in LUAD, the 5-year survival rate of LUAD patients has been somewhat improved, especially with immunotherapy drug applications such as the programmed cell death protein 1/ programmed cell death protein ligand 1 (PD-1/PD-L1). There are new challenges, and the response rate of some patients to immunotherapy is not high [3, 4]. It is imperative to identify new biomarkers to predict the curative effect of immunotherapy
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