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首页> 外文期刊>Metabolic brain disease >Loss of PPAR alpha perpetuates sex differences in stroke reflected by peripheral immune mechanisms
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Loss of PPAR alpha perpetuates sex differences in stroke reflected by peripheral immune mechanisms

机译:PPARα的丧失使周围性免疫机制反映出的中风性别差异永久存在

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摘要

Peroxisome proliferator-activated receptor alpha (PPAR alpha) is a nuclear receptor transcription factor that plays a role in immune regulation. Because of its expression in cerebral tissue and immune cells, PPAR alpha has been examined as an important regulator in immune-based neurological diseases. Many studies have indicated that pre-treatment of animals with PPAR alpha agonists induces protection against stroke. However, our previous reports indicate that protection is only in males, not females, and can be attributed to different PPAR alpha expression between the sexes. In the current study, we examine how loss of PPAR alpha affects male and female mice in experimental stroke. Male and female PPAR alpha knockout mice were subject to middle cerebral artery occlusion (MCAO) or sham surgery, and the ischemic (local) or spleen specific (peripheral) immune response was examined 96 h after reperfusion. We found that loss of PPAR alpha perpetuated sex differences in stroke, and this was driven by the peripheral, not local, immune response. Specifically we observed an increase in peripheral pro-inflammatory and adhesion molecule gene expression in PPAR alpha KO males after MCAO compared to females. Our data supports previous evidence that PPAR alpha plays an important role in sex differences in the immune response to disease, including stroke.
机译:过氧化物酶体增殖物激活受体α(PPAR alpha)是一种核受体转录因子,在免疫调节中起作用。由于其在脑组织和免疫细胞中的表达,PPARα已被检测为基于免疫的神经系统疾病的重要调节剂。许多研究表明,用PPARα激动剂对动物进行预处理可诱导预防中风。但是,我们以前的报告表明,保护仅在男性中,而不在女性中,并且可以归因于性别之间不同的PPAR alpha表达。在当前的研究中,我们检查了PPARα的损失如何影响实验性卒中中的雄性和雌性小鼠。对雄性和雌性PPARα基因敲除小鼠进行大脑中动脉闭塞(MCAO)或假手术,并在再灌注后96小时检查缺血性(局部)或脾脏特异性(外周)免疫反应。我们发现,PPARα的丧失使中风的性别差异永存,这是由外周而非局部免疫反应驱动的。具体而言,我们观察到与女性相比,MCAO后男性中PPAR alpha KO男性的外周促炎和粘附分子基因表达增加。我们的数据支持以前的证据,即PPARα在对包括中风在内的疾病的免疫反应中的性别差异中起着重要作用。

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