The Key Laboratory of Cardiovascular Remodeling and Function Research, Chinese Ministry of Education, Chinese Ministry of Health and Chinese Academy of Medical Sciences, Qilu Hospital of Shandong University, Jinan, China.
Department of Pharmacy, Jinan Central Hospital Affiliated to Shandong University, Jinan, China.
Int J Cardiol. 2018 Jul 15;263:96-103. doi: 10.1016/j.ijcard.2018.04.018. Epub 2018 Apr 7.
It remains unknown whether Non-POU-domain-containing octamer-binding protein (NonO) plays a causative role in plaque destabilization. We hypothesized that NonO gene silencing may stabilize atherosclerotic plaque by increasing P4Hα1 expression and inhibiting the inflammation.
Vulnerable atherosclerotic plaques were induced in ApoE-/- mice by high fat diet, perivascular collar placement and mental stress. Compared with normal carotid arteries, those contained vulnerable plaques had high NonO expression. In another in vivo experiment, mice contained vulnerable plaques were randomly divided into 5 groups to receive physiological saline, si-N.C-lentivirus (LV), si-NonO-LV, pGC-GFP-LV and NonO-LV, respectively. NonO overexpression increased while NonO silencing decreased the incidence of carotid plaque disruption. NonO overexpression enhanced macrophage infiltration and lipid deposition but reduced the content of vascular smooth muscle cells and collagen in plaques, leading to an increased plaque vulnerability index, whereas NonO silencing exhibited the opposite effect. In addition, NonO overexpression increased the expression of proinflammatory cytokines and matrix metalloproteinases and decreased the expression of P4Hα1 both in vivo and in vitro, whereas NonO silencing showed the contrary effect. NonO co-immunoprecipitated with NF-κB p65, and promoted its nuclear translocation and phosphorylation, and these effects were reversed by NonO silencing.
NonO may promote plaque destabilization and increase the incidence of plaque disruption in ApoE-/- mice by inducing the expression of inflammatory cytokines and matrix metalloproteinases and suppressing that of P4Hα1. The mechanism may involve the interaction of NonO with NF-κB leading to enhanced NF-κB nuclear translocation and phosphorylation.
目前尚不清楚非 POU 域结合八聚体结合蛋白(NonO)是否在斑块不稳定中起致病作用。我们假设 NonO 基因沉默可能通过增加 P4Hα1 表达和抑制炎症来稳定动脉粥样硬化斑块。
通过高脂肪饮食、血管周袖套放置和精神压力在 ApoE-/- 小鼠中诱导易损性动脉粥样硬化斑块。与正常颈动脉相比,易损斑块中含有高表达的 NonO。在另一个体内实验中,将含有易损斑块的小鼠随机分为 5 组,分别接受生理盐水、si-N.C-慢病毒(LV)、si-NonO-LV、pGC-GFP-LV 和 NonO-LV。NonO 过表达增加,而 NonO 沉默减少颈动脉斑块破裂的发生率。NonO 过表达增强了巨噬细胞浸润和脂质沉积,但减少了斑块中血管平滑肌细胞和胶原的含量,导致斑块易损指数增加,而 NonO 沉默则表现出相反的效果。此外,NonO 过表达增加了体内和体外促炎细胞因子和基质金属蛋白酶的表达,降低了 P4Hα1 的表达,而 NonO 沉默则表现出相反的效果。NonO 与 NF-κB p65 共免疫沉淀,并促进其核转位和磷酸化,而 NonO 沉默则逆转了这些作用。
NonO 通过诱导促炎细胞因子和基质金属蛋白酶的表达,抑制 P4Hα1 的表达,可能促进 ApoE-/- 小鼠斑块不稳定,增加斑块破裂的发生率。其机制可能涉及 NonO 与 NF-κB 的相互作用,导致 NF-κB 核转位和磷酸化增强。
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