Major vault protein inhibits apoptosis of aortic endothelial cells through upregulating interferon regulatory factor 2
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R329.25

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    Abstract:

    Objective:To investigate the effects and the underlying mechanism of major vault protein(MVP)on the proliferation of arterial endothelial cells. Methods:Human aortic endothelial cell(HAEC)were infected with lentivirus to inhibit or overexpress MVP. Cell proliferation and death were detected with CCK-8 assay and flow cytometry. Apoptosis inhibitor Z-VAD and necroptosis inhibitor Nec-1 were used to distinguish the mode of cell death. Annexin V binding and Caspase 3 activity were detected by flow cytometry,and cleaved Caspase was examined by Western blot. Real time PCR and Western blot were performed to investigate target molecules and the regulatory relationship. Results:Knockdown of MVP inhibited the proliferation activity of HAEC and promoted the HAEC cell death. Overexpression of MVP resulted in the opposite results. Treatment with Z-VAD reversed HAEC death caused by MVP knockdown,while Nec-1 did not. Consistently,TNF-α-induced HAEC apoptosis was inhibited by MVP overexpression and exaggerated by MVP knocked down. MVP promoted the transcriptional expression of cellular inhibitor of apoptosis proteins1(cIAP1)by up-regulating interferon regulatory factor 2(IRF2)protein expression. IRF2 knockdown reversed the increase in cIAP1 expression and the decrease in apoptosis caused by MVP overexpression. Conclusion:MVP promoted cIAP1 transcription by up-regulating IRF2 protein expression,thereby inhibiting TNF-α-induced apoptosis and promoting the proliferation of arterial EC.

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薛佳佳,王艺颖,胡成秀,孙崇秀.穹窿主体蛋白通过上调干扰素调节因子2抑制动脉内皮细胞凋亡[J].南京医科大学学报(自然科学版英文版),2023,(8):1076-1084.

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  • Received:January 30,2023
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  • Online: August 10,2023
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