GPR37 expression as a prognostic marker in gliomas: a bioinformatics-based analysis

Kairong Liang; Zhaoxiong Guo; Shizhen Zhang; Danmin Chen; Renheng Zou; Yuhao Weng; Chengxiang Peng; Zhichao Xu; Jingbai Zhang; Xiaorui Liu; Xiao Pang; Yunxiang Ji; Degui Liao; Miaoling Lai; Huaidong Peng; Yanbin Ke; Zhaotao Wang; Yezhong Wang

doi:doi:10.18632/aging.205063

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Research Paper Volume 15, Issue 19 pp 10146—10167

GPR37 expression as a prognostic marker in gliomas: a bioinformatics-based analysis

Figure 6. (A) GSEA results showing differential enrichment of GO terms as a function of GPR37 expression. Top 5 GO terms for GPR37^high- positive regulation of macrophage derived foam cell differentiation, negative regulation of T cell receptor signaling pathway, leukocyte proliferation, B cell proliferation and myeloid leukocyte differentiation. Top 5 GO terms for GPR37^low- immunoglobulin complex, immunoglobulin complex circulating, antigen binding, immunoglobulin receptor binding and humoral immune response mediated by circulating immunoglobulin. (B) GSEA results showing differential enrichment of KEGG pathways as a function of GPR37. Top 5 KEGG pathways for GPR37^high-neuroactive ligand receptor interaction, calcium signaling pathway, B cell receptor signaling pathway, PPAR signaling pathway and toll like receptor signaling pathway. Two KEGG pathways in GPR37^low- ribosome, spliceosome and oxidative phosphorylation. All results of GSEA were based on NES, adjusted P value and FDR value. GSEA, gene set enrichment analysis.