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Role of IGFBP1 in the senescence of vascular endothelial cells and severity of aging-related coronary atherosclerosis

机译:IGFBP1在血管内皮细胞衰老和衰老相关性冠状动脉粥样硬化严重程度中的作用

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摘要

The senescence of vascular endothelial cells (ECs) plays a critical role in aging-related cardiovascular diseases. We previously reported the causal relation of Jagged1 in ECs and the thickening of the arterial wall in aging mice. The aim of the present study was to further investigate the correlation between insulin-like growth factor-binding protein 1 (IGFBP1), one of the secretory proteins regulated by Jagged1, and the severity of coronary atherosclerosis and patient age, as well as its effect on EC senescence. First, microarray analysis was performed to screen the differentially expressed genes regulated by Jagged1 in human coronary arterial ECs (HCAECs). Inhibition of the Jagged1 expression using a small interfering RNA knockdown method in HCAECs led to the upregulation of 17 and the downregulation of 78 genes by >3-fold, and IGFBP1 was confirmed to be a secretory protein expressed by HCAECs and regulated by Jagged1. Subsequently, in 112 consecutively enrolled patients with acute chest pain who underwent coronary angiography, the circulating level of IGFBP1 was found to be positively correlated with age (r=0.512, P<0.001) and Synergy between PCI with TAXUS and Cardiac Surgery (SYNTAX) score (r=0.409, P<0.001). Among age-comparable patients, the circulating IGFBP1 level was found to be increased in patients with higher SYNTAX scores. In cultured HCAECs, IGFBP1 was shown to protect ECs against passage- or H2O2-induced senescence, and these protective effects of IGFBP1 may be partially reversed by , a known Akt signaling inhibitor. Therefore, the results of the present study suggested that, as a downstream protein of Jagged1, IGFBP1 was correlated with the severity of coronary atherosclerosis in aging patients, and the increase of circulating IGFBP1 levels with aging may be an adaptive response to counter HCAEC senescence through Akt signaling.
机译:血管内皮细胞(EC)的衰老在与衰老相关的心血管疾病中起着至关重要的作用。我们先前报道了ECs中Jagged1的因果关系以及衰老小鼠中动脉壁的增厚。本研究的目的是进一步研究胰岛素样生长因子结合蛋白1(IGFBP1)(由Jagged1调节的一种分泌蛋白)与冠状动脉粥样硬化的严重程度,患者年龄及其影响之间的相关性。 EC衰老。首先,进行微阵列分析以筛选人冠状动脉EC(HCAEC)中受Jagged1调控的差异表达基因。在HCAEC中使用小干扰RNA敲低方法抑制Jagged1表达可导致17个上调和78个基因的下调> 3倍,并且IGFBP1被证实是HCAECs表达的分泌蛋白,并受Jagged1调控。随后,在112例接受了冠脉造影的连续入选的急性胸痛患者中,IGFBP1的循环水平与年龄(r = 0.512,P <0.001)以及PCI与TAXUS和心脏外科手术之间的协同作用(SYNTAX)呈正相关。得分(r = 0.409,P <0.001)。在年龄可比的患者中,发现SYNTAX评分较高的患者循环IGFBP1水平升高。在培养的HCAEC中,IGFBP1被证明可以保护EC免受传代或H2O2诱导的衰老,而IGFBP1的这些保护作用可能会被已知的Akt信号抑制剂部分逆转。因此,本研究结果表明,IGFBP1作为Jagged1的下游蛋白,与衰老患者的冠状动脉粥样硬化的严重程度相关,并且随着年龄的增长,循环中IGFBP1水平的升高可能是通过逆转HCAEC衰老的适应性反应。 Akt信令。

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