Introduction
The abnormal changes in genes have been proved to participate in the occurrence and development of cancer. Exploring the cancer-related genes and their signaling pathways by pan-cancer analysis could contribute to the diagnosis and clinical treatment of human cancers [
1,
2].
Lymphocyte-activation gene 3 (LAG3) is located on chromosome 12 (12p13.32) and encodes a type 1 transmembrane protein involved in tumor immune regulation and clinical aggressiveness [
3,
4]. It is widely expressed on various immune cells, predominantly found on the surface of diverse T lymphocytes including CD4 + and CD8 + subsets, as well as other immune cell populations [
5]. As an inhibitory receptor, LAG3 exerts its influence on tumor progression by modulating T cell activation and effector function [
6]. However, as an immunosuppressive receptor, there is a complex interplay between LAG3 and the infiltration and functionality of immune cells. In breast cancer, elevated levels of LAG3 expression have been positively associated with multiple immune cell infiltrates [
7]. The immunohistochemical staining in gastric cancer reveals a positive correlation between an increased number of LAG3-positive cells and patient prognosis [
8]. Furthermore, LAG3 can also stimulate mature dendritic cells (DCs) to produce cytokines such as IL-12 and TNF-a [34067904]. Notably, the emerging animal experiments and clinical trials have demonstrated that blockade of LAG3 enhances the anti-tumor efficacy, underscoring its potential in cancer therapy [
9‐
11]. Given the intricate expression pattern of LAG3 across different cancers, comprehensive exploration of this receptor from a pan-cancer perspective is imperative.
In this study, we comprehensively assessed the characteristics of LAG3 in various cancer types using a range of bioinformatics platforms. We conducted comparative analyses of differential expression profiles and gene alterations of LAG3 between cancer and normal tissues, and evaluated their prognostic significance on the prognostic values and immune responses.
Materials and methods
Gene expression analysis
We conducted an analysis of LAG3 expression profiles between tumor tissues and normal tissues using Tumor Immune Estimation Resource 2.0 (TIMER2.0). We utilized the Gene Expression Profiling Interactive Analysis 2 (GEPIA2) database to investigate the relationship between LAG3 expression and the pathological stage of TCGA tumors.
Immumohistochemical staining
20 pairs of paraffin-embedded tissues from patients diagnosed with cutaneous malignant melanoma or non-specific skin inflammation were included. The LAG3 rabbit-derived polyclonal antibody from Proteintech Group (29,548-1-AP) was utilized with a dilution ratio of 1:4000 for this experiment.
Genetic alteration evaluation
The cBio Cancer Genomics Portal (cBioPortal) an interactive algorithm containing multidimensional cancer genomics datasets, was employed to investigate the molecular profiles and clinical attributes of pan-cancer samples in terms of genomics. In this study, the cBioPortal platform was utilized to evaluate the genetic alterations of LAG3 in TCGA cancers, including the types of genetic alteration and mutation sites.
Survival analysis
The prognostic value of LAG3 expression in multiple cancers was assessed using the GEPIA2 database. Additionally, the cBioPortal platform was utilized to determine the survival significance of LAG3 genetic alterations in cancer patients, encompassing overall survival (OS), disease-free survival (DFS), disease-specific survival (DSS) and progression-free survival (PFS).
Immune infiltration analysis
The TIMER2.0 software was employed to investigate the correlation between LAG3 expression and various tumor-infiltrating immune cells populations, including B cells, CD8 + T cells, DCs, macrophages, neutrophils, natural killer cells (NK cells) and monocytes. Furthermore, the Gene Set Enrichment Analysis (GSEA) algorithm available at Xiantao XueShu (
https://www.xiantao.love/products) was utilized to validate the roles of LAG3 in the regulation of immune-associated signaling pathways.
LAG3-associated gene enrichment analysis
The STRING was utilized to construct the LAG3-associated molecule network. We applied the GEPIA2 database to investigate the top 100 LAG3-related molecules in TCGA pan-cancer dataset. Subsequently, Pearson correlation analysis was performed to assess the relationship between LAG3 and the top 6 LAG3-related molecules across various cancer types. GSEA enrichment analysis was conducted to elucidate the underlying biological functions of LAG3 in cancer progression.
Single-cell level assessment of LAG3 expression
We analyzed the single-cell distribution patterns and biological functions of LAG3 using CancerSEA tool [
16]. The Tumor Immunity Single Cell Center (TISCH) [
17] is a scRNA-seq database specifically dedicated to investigating the tumor microenvironment (TME). We also employed TISCH database to investigate the expression pattern of LAG3 in SKCM at single-cell level.
Discussion
LAG3, locating on chromosome 12 (12p13.32) and encoding a type 1 transmembrane protein, has been proved to be involved in immune regulation and clinical aggressiveness of cancer [
18]. In breast cancer and lung adenocarcinoma, the high expression of LAG3 is closely related to the increase of T cell infiltration [
7]. LAG3 could also directly and competitively bind with pHLA-II, to inhibiting T cell activation by affecting the combination of CD4 and pHLA-II [
19]. Here, we performed a comprehensive analysis of LAG3 through multiple bioinformatics platforms to explore the functional roles of LAG3 in pan-cancer.
Based on the TCGA database, we investigated the expression of LAG3 in 33 cancers. We noticed that LAG3 was upregulated in most cancers, including BRCA, ESCA, GBM, HNSC, KIRC, LUAD, LURC, PCPG and STAD. Conversely, LAG3 was downregulated in COAD, KICH, LIHC, PRAD, READ, THCA and UCEC. Meanwhile, GEPIA2 database proved that in ACC, KIRC, COAD and OV, LAG3 expression was consistent with the pathological stage of patients. Then, Kaplan–Meier plotter showed that OV and UCEC patients with high LAG3 expression had better OS and RFS, while KIRC patients with high LAG3 expression had worse prognosis. These results suggest that the aberrantly expressed LAG3 could be a potential predictor for the prognosis of UCEC and OV cancer patients, and can assist in clinic pathological staging.
In addition, we also proved that the expression of LAG3 was significantly related with immune cell infiltration, including macrophage, CD8 + T cells, B cells, DCs, macrophage and NK cells. In earlier studies, LAG3 was a negative regulator of T cell activation and function [
20]. Blocking the effect of LAG3 on human CD4 clones leads to increased production of IL-2, IL-4, IFN-γ, and TNF-α [
21]. In mouse models of ovarian cancer, co-blocking LAG3 and PD-1 expressed on CD4 + and CD8 + TILs induces enhanced anti-tumor response [
6]. Recent studies have shown that the combination of T cell checkpoint 41BB agonist and LAG3 antagonist could improve the anti-tumor immunity in pancreatic cancer [
11]. Increased expression of LAG3 driven by IL6 led to decreased function of peripheral CD8 + T cells and reduced tumor therapeutic resistance [
22]. Other studies also confirmed the regulatory roles of highly expressed LAG3 in the tumor infiltration of immune cells, including T cells, B cells, NK cells and DCs [
23]. These results suggested the significant regulatory roles of LAG3 in the regulation of immune response.
Recent studies showed that high expression of LAG3 predicts a poor prognosis in patients due to its promotion of immune escape [
24]. However, in SKCM, high expression of LAG3 suggests a favorable prognosis. These positive effects may be attributed to LAG3-mediated hyperactivation of immune system in SKCM [
25,
26]. The discovery highlights the potential of LAG3 as a biomarker for assessing the immune system status in patients with SKCM, thereby offering valuable insights for its therapeutic management.
Conclusions
In conclusion, this is the first extensive research about the expression profiles, prognostic values, and functional significance of LAG3 in human pan-cancers. We demonstrate that LAG3 may be a novel prognostic marker for OV and UCEC. In addition, LAG3 expression could be associated with the tumor-infiltrating immune cells and might be an underlying predictive biomarker for cancer immunotherapeutic response. These results proved that LAG3 was closely related to tumor pathogenesis and immune response.
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