A Methylation-Based Reclassification of Bladder Cancer Based on Immune Cell Genes

A Methylation-Based Reclassification of Bladder Cancer Based on Immune Cell Genes

Simple Summary Bladder cancer (BC) development is highly related to immune cell infiltration. In this study, we aimed to construct a new classification of bladder cancer molecular subtypes based on immune-cell-associated CpG(Methylation) sites. The classification was accurate and stable. BC patients...

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Veröffentlicht in:Cancers 2020-10, Vol.12 (10), p.3054, Article 3054
Hauptverfasser: Luo, Qizhan, Vogeli, Thomas-Alexander
Format: Artikel
Sprache:eng
Schlagworte:
Adenomatous polyposis coli
Biomarkers
Bladder cancer
Cancer
Cancer therapies
Chemotherapy
Classification
CpG islands
Diagnosis
DNA methylation
Drug therapy
FDA approval
Gene expression
Genetic aspects
Genomics
Health aspects
Histocompatibility antigen HLA
Immune system
Immunotherapy
Infiltration
Interferon
Life Sciences & Biomedicine
Major histocompatibility complex
Medical prognosis
Metastases
Metastasis
Methylation
Microenvironments
Mutation
Oncology
Principal components analysis
Prognosis
Reclassification
Science & Technology
Tumors
Vaccines
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Zusammenfassung:Simple Summary Bladder cancer (BC) development is highly related to immune cell infiltration. In this study, we aimed to construct a new classification of bladder cancer molecular subtypes based on immune-cell-associated CpG(Methylation) sites. The classification was accurate and stable. BC patients were successfully divided into three subtypes based on the immune-cell-associated CpG sites. The clinicopathologic features, distribution of immune cells, level of expression of checkpoints, stromal score, immune score, ESTIMATEScore, tumor purity, APC co_inhibition, APC co_stimulation, HLA, MHC class_I, Type I IFN_respons, Type II IFN response, and DNA stemness score (DNAss) presented significant differences among the three subgroups. The specific genomic alteration was also different across subgroups. High-level immune infiltration showed a correlation with high-level methylation. A lower RNA stemness score (RNAss) was associated with higher immune infiltration. Cluster 2 demonstrated a better response to chemotherapy. The anti-cancer targeted drug therapy results are different among the three subgroups. Background: Bladder cancer is highly related to immune cell infiltration. This study aimed to develop a new classification of BC molecular subtypes based on immune-cell-associated CpG sites. Methods: The genes of 28 types of immune cells were obtained from previous studies. Then, methylation sites corresponding to immune-cell-associated genes were acquired. Differentially methylated sites (DMSs) were identified between normal samples and bladder cancer samples. Unsupervised clustering analysis of differentially methylated sites was performed to divide the sites into several subtypes. Then, the potential mechanism of different subtypes was explored. Results: Bladder cancer patients were divided into three groups. The cluster 3 subtype had the best prognosis. Cluster 1 had the poorest prognosis. The distribution of immune cells, level of expression of checkpoints, stromal score, immune score, ESTIMATEScore, tumor purity, APC co_inhibition, APC co_stimulation, HLA, MHC class_I, Type I IFN Response, Type II IFN Response, and DNAss presented significant differences among the three subgroups. The distribution of genomic alterations was also different. Conclusions: The proposed classification was accurate and stable. BC patients could be divided into three subtypes based on the immune-cell-associated CpG sites. Specific biological signaling pathways, immune mechanis
ISSN:2072-6694
2072-6694
DOI:10.3390/cancers12103054