摘要:SummaryEndometrial angiogenesis is necessary for good endometrial receptivity. Krüppel-like factor 4 (KLF4) is a transcription factor that is essential for regulating angiogenesis. Here we found that vascular endothelial growth factor A (VEGFA) can form a positive feedback loop with KLF4 to promote the proliferation and migration of human endometrial microvascular endothelial cells (HEMECs) and inhibit cell apoptosis. General control non-derepressible 5 (GCN5) is also time-dependent on VEGFA and participates in the KLF4-VEGFA loop. In addition, we found that GCN5 is a succinyltransferase that modulates the succinylation of histones and nonhistones. GCN5 interacts with KLF4 and is recruited to the KLF4-binding site of the VEGFA promoter to succinylate H3K79, which initiates gene transcription epigenetically. For nonhistones, GCN5 succinylates KLF4 that is activated by ERK signaling in HEMECs treated with VEGFA to increase its transcription activity. These results demonstrate KLF4-VEGFA positive feedback loop is regulated by epigenetics, which contributes to endometrial angiogenesis.Graphical abstractDisplay OmittedHighlights•KLF4 mediates VEGFA-induced endometrial angiogenesis•VEGFA increases the interaction between KLF4 and GCN5•VEGFA promotes H3K79 succinylation by upregulating KLF4 and GCN5•VEGFA succinylates KLF4 and promotes interaction of KLF4 and GCN5 via ERK pathwayBiological sciences; Molecular biology; Cell biology;
