Implications of the KHDC4-TRAF2 axis in the context of prostate cancer prognosis

Su-Wei Hu; Chia-Chang Wu; Shao-Wei Dong; Kai-Yi Tzou; Chih-Heng Chen; Yuan-Hung Wang; Yen-Nien Liu; Chiao-Chun Liao; Chien-Hsiu Li

doi:doi:10.18632/aging.206273

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Research Paper Volume 17, Issue 6 pp 1544—1570

Implications of the KHDC4-TRAF2 axis in the context of prostate cancer prognosis

Figure 4. Shared gene ontology between TRAF2 and KHDC4 is associated with adverse prognosis outcomes. (A) A Venn diagram analysis collecting molecules positively or negatively correlated to TRAF2 in TCGA-PRAD datasets (Cell 2015, Firehose Legacy, and PanCancer Atlas). (B) Graphical abstract illustrating the potential biological roles influenced by TRAF2 in prostate cancer. (C) Canonical pathways affected by TRAF2-related molecules. (D) Molecular links to TRAF2 regulations in prostate cancer. (E) The correlation of KHDC4 and TRAF2 individually with Progression-Free Interval (PFI) and Disease-Free Interval (DFI) in TCGA-PRAD. (F) The correlation of Progression-Free Interval (PFI) and Disease-Free Interval (DFI) in TCGA-PRAD with the combined distribution of KHDC4 and TRAF2.