Smurf2-Mediated Ubiquitination of FOXO4 Regulates Oxygen-glucose Deprivation/Reperfusion-induced Pyroptosis of Cortical Neurons.

Bin Yan, Yan Jin, Song Mao, Yi Zhang, Dahong Yang, Mingyang Du, Yugang Yin
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Abstract

Background: Smad ubiquitination regulatory factor 2 (Smurf2) has been observed to alleviate ischemia-reperfusion injury. This study sought to explore the molecular mechanism of Smurf2-mediated forkhead box O4 (FOXO4) ubiquitination in oxygen-glucose deprivation/ reperfusion (OGD/R)-induced pyroptosis of cortical neurons.

Methods: Human cortical neurons (HCN-2) were subjected to OGD/R to establish a cell model of cerebral stroke. Smurf2, FOXO4, and doublecortin domain containing 2 (DCDC2) expressions were determined by RT-qPCR and Western blot. LDH release, pyroptosis-related proteins NLRP3, GSDMD-N, and cleaved-caspase-3, as well as inflammatory factors IL-1β and IL-18, were assessed by LDH assay kit, Western blot, and ELISA. The ubiquitination level of FOXO4 was determined by ubiquitination assay. The bindings of Smurf2 to FOXO4 and FOXO4 to DCDC2 were testified by Co-IP, ChIP, and dual-luciferase assays. Rescue experiments were designed to validate the role of FOXO4/DCDC2 in the pyroptosis of HCN-2 cells.

Results: Smurf2 was weakly expressed, while FOXO4 and DCDC2 were prominently expressed in OGD/R-treated HCN-2 cells. Smurf2 overexpression promoted LDH release, reduced NLRP3, GSDMD-N, and cleaved-caspase-3 proteins, and decreased IL-1β and IL-18 concentrations. Sumrf2 improved the ubiquitination level of FOXO4 to downregulate its protein level. FOXO4 is bound to the DCDC2 promoter to facilitate its transcription. Overexpression of FOXO4 or DCDC2 reversed the inhibition of Smurf2 overexpression on pyroptosis of OGD/Rtreated HCN-2 cells.

Conclusion: Smurf2 overexpression facilitated the ubiquitination of FOXO4 to reduce its protein level, thereby suppressing DCDC2 transcription and restricting OGD/R-induced pyroptosis of cortical neurons.

Smurf2介导的FOXO4泛素化调节氧-葡萄糖剥夺/再灌注诱导的皮质神经元Pyroptosis。
背景:Smad泛素化调节因子2(Smurf2)已被观察到可减轻缺血再灌注损伤。本研究旨在探讨蓝精灵介导的叉头盒O4(FOXO4)泛素化在氧-葡萄糖剥夺/再灌注(OGD/R)诱导的皮层神经元焦下垂中的分子机制。方法:将人皮质神经元(HCN-2)进行OGD/R,建立脑卒中细胞模型。通过RT-qPCR和蛋白质印迹测定Smurf2、FOXO4和双皮质素结构域含2(DCDC2)的表达。LDH释放、pyroptosis相关蛋白NLRP3、GSDMD-N和裂解的胱天蛋白酶-3,以及炎症因子IL-1β和IL-18,通过LDH测定试剂盒、Western印迹和ELISA进行评估。FOXO4的泛素化水平通过泛素化测定法测定。通过Co-IP、ChIP和双荧光素酶测定证实了Smurf2与FOXO4和FOXO4与DCDC2的结合。救援实验旨在验证FOXO4/DCDC2在HCN-2细胞焦下垂中的作用。结果:在OGD/R处理的HCN-2细胞中,Smurf2弱表达,而FOXO4和DCDC2显著表达。Smurf2过表达促进LDH释放,降低NLRP3、GSDMD-N和裂解的胱天蛋白酶-3蛋白,并降低IL-1β和IL-18浓度。Sumrf2提高FOXO4的泛素化水平以下调其蛋白质水平。FOXO4与DCDC2启动子结合以促进其转录。FOXO4或DCDC2的过表达逆转了Smurf2过表达对OGD/R处理的HCN-2细胞焦下垂的抑制作用。结论:Smurf2过表达促进了FOXO4的泛素化,降低了其蛋白水平,从而抑制了DCDC2的转录,限制了OGD/R诱导的皮层神经元焦下垂。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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