Multi-omics approaches establishing histone modification based prognostic model in glioma patients and further verification of the carcinogenesis mechanism

Yunhui Wang; LiKang Ji; Chunfeng Ji; Fan Wang

doi:10.1007/s10142-023-01229-3

Multi-omics approaches establishing histone modification based prognostic model in glioma patients and further verification of the carcinogenesis mechanism

Funct Integr Genomics. 2023 Sep 21;23(4):307. doi: 10.1007/s10142-023-01229-3.

Authors

Yunhui Wang¹, LiKang Ji¹, Chunfeng Ji¹, Fan Wang²

Affiliations

¹ Department of Neurosurgery, Deqing People's Hospital, Deqing, Zhejiang Province, China.
² Department of Neurosurgery, The First Affiliated Hospital of Wenzhou Medical University, Ouhai, Wenzhou, Zhejiang, 325000, China. wangfan@wmu.edu.cn.

PMID: 37730879
DOI: 10.1007/s10142-023-01229-3

Abstract

Glioblastoma (GBM) emerges as the most common malignant brain tumor. Histone modifications, as an epigenetic regulatory mechanism of gene expression, are closely associated with malignant tumors. Gene set related to histone modification was extracted from the MSigDB database, and scored by the function of AddModuleScore. Pearson correlation analysis was utilized using the "rcorr" function of "Hmisc" R package. Genes were screened out using the LASSO Cox analysis. TCGA-GBM and CGGA_array_301 cohorts were employed for constructing model and validation. We calculated immune infiltration scores using microenvironment cell populations counter (MCPcounter), single-sample gene set enrichment analysis (ssGSEA), and xCell algorithms. U87-MG and CHG-5 cell lines were utilized to evaluate expression level of TMEM176A by western blot (WB). Transwell, EDU, colony formation analysis (CFA), and CKK-8 assays were conducted to investigate cell proliferation and migration rate. The malignant cells in GBM patients exhibited notable activation in the TGF-β and hypoxia pathway. Histone modifications were associated with adhesion and neuron development in GBM. We identified a model with five significant genes, namely NBEAL1, AEBP1, TMEM176A, FASTK, and CD81, with prognostic efficacy. Additionally, we observed increased infiltration of T cells and CD8+ T cells in the high-risk (HR) group. 5-Fluorouracil_1073 and Taselisib_1561 were predicted as potential treatment options for GBM patients, while ABT737_1910 and Wnt_C59-1622 exhibited superior response in GBM patients of the HR group. A spike in the TP53 mutation rate was observed in the HR group. TMEM176A played a role in regulating cell proliferation and migration in vitro. We presented a novel prognostic model for patients with GBM, based on histone modification-related genes. In addition, we identified the crucial role of the TMEM176A in the regulation of GBM carcinogenic phenotypes for the first time.

Keywords: Glioblastoma; Histone modification; Prognosis; TMEM176A.

MeSH terms

Carboxypeptidases
Carcinogenesis
Glioma*
Histone Code*
Histones / genetics
Humans
Membrane Proteins
Multiomics
Prognosis
Protein Serine-Threonine Kinases
Repressor Proteins
Tumor Microenvironment

Substances

Histones
AEBP1 protein, human
Carboxypeptidases
Repressor Proteins
TMEM176A protein, human
Membrane Proteins
FASTK protein, human
Protein Serine-Threonine Kinases