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首页> 美国卫生研究院文献>other >Cardiac Overexpression of Alcohol Dehydrogenase Exacerbates Chronic Ethanol Ingestion-Induced Myocardial Dysfunction and Hypertrophy: Role of Insulin Signaling and ER stress
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Cardiac Overexpression of Alcohol Dehydrogenase Exacerbates Chronic Ethanol Ingestion-Induced Myocardial Dysfunction and Hypertrophy: Role of Insulin Signaling and ER stress

机译:酒精脱氢酶的心脏过度表达加剧了慢性乙醇摄入引起的心肌功能障碍和肥大:胰岛素信号和内质网应激的作用

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Chronic alcohol intake leads to alcoholic cardiomyopathy characterized by cardiac hypertrophy and contractile dysfunction possibly related to the toxicity of the ethanol metabolite acetaldehyde. This study examined the impact of augmented acetaldehyde exposure on myocardial function, geometry, and insulin signaling via cardiac-specific overexpression of alcohol dehydrogenase (ADH). ADH transgenic and wild-type FVB mice were placed on a 4% alcohol diet for 12 wks. Echocardiographic, glucose tolerance, glucose uptake, insulin signaling, and ER stress indices were evaluated. Mice consuming alcohol exhibited glucose intolerance, dampened cardiac glucose uptake, cardiac hypertrophy and contractile dysfunction, all of which with the exception of whole body glucose tolerance were exaggerated by the ADH transgene. Cardiomyocytes from ethanol-fed mice exhibited depressed insulin-stimulated phosphorylation insulin receptor (tyr1146) and IRS-1 (tyrosine) as well as enhanced serine phosphorylation of IRS-1. ADH augmented alcohol-induced effect of IRS-1 phosphorylation (tyrosine/serine). Neither alcohol nor ADH affected expression of insulin receptor and IRS-1. Alcohol reduced phosphorylation of Akt and GSK-3β as well as GSK-3β expression and the effect was exaggerated by ADH. The transcriptional factors GATA4, c-Jun and c-Jun phosphorylation were upregulated by alcohol, which was amplified by ADH. The ratios of phospho-c-Jun/c-Jun and phospho-GATA4/GATA4 remained unchanged. Chronic alcohol intake upregulated expression of the endoplasmic reticulum stress markers eIF2α, IRE-1α, GRP78 and gadd153, the effect of which was exaggerated by ADH. These data suggest that elevated cardiac acetaldehyde exposure via ADH may exacerbate alcohol-induced myocardial dysfunction, hypertrophy, insulin insensitivity and ER stress, indicating a key role of ADH gene in alcohol-induced cardiac dysfunction and insulin resistance.
机译:长期摄入酒精会导致酒精性心肌病,其特征在于心脏肥大和收缩功能障碍,可能与乙醇代谢物乙醛的毒性有关。这项研究通过心脏特异性乙醇脱氢酶(ADH)的过表达,研究了乙醛暴露量增加对心肌功能,几何形状和胰岛素信号传导的影响。将ADH转基因和野生型FVB小鼠置于4%酒精饮食中12周。评估了超声心动图,葡萄糖耐量,葡萄糖摄取,胰岛素信号传导和内质网应激指数。饮酒的小鼠表现出葡萄糖耐量下降,心脏葡萄糖摄取减弱,心脏肥大和收缩功能障碍,除全身葡萄糖耐量外,所有这些都被ADH转基因夸大了。用乙醇喂养的小鼠的心肌细胞表现出胰岛素刺激的磷酸化胰岛素受体(tyr1146)和IRS-1(酪氨酸)降低,以及IRS-1的丝氨酸磷酸化增强。 ADH增强了酒精诱导的IRS-1磷酸化(酪氨酸/丝氨酸)的作用。酒精和ADH均不影响胰岛素受体和IRS-1的表达。酒精会降低Akt和GSK-3β的磷酸化以及GSK-3β的表达,ADH会放大这种作用。转录因子GATA4,c-Jun和c-Jun磷酸化被酒精上调,并被ADH扩增。磷酸-c-Jun / c-Jun和磷酸-GATA4 / GATA4的比例保持不变。慢性酒精摄入会上调内质网应激标志物eIF2α,IRE-1α,GRP78和gadd153的表达,ADH会放大其作用。这些数据表明,通过ADH暴露的心脏乙醛暴露升高可能加剧酒精诱导的心肌功能障碍,肥大,胰岛素不敏感性和内质网应激,表明ADH基因在酒精诱导的心脏功能障碍和胰岛素抵抗中起关键作用。

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