Heneka Michael T, Landreth Gary E
Department of Neurology, Molecular Neurology Unit, Mendelstrasse 7, University of Münster, Albert Schweitzer-Strasse 33, 48149 Münster, Germany.
Biochim Biophys Acta. 2007 Aug;1771(8):1031-45. doi: 10.1016/j.bbalip.2007.04.016. Epub 2007 May 10.
The biology of peroxisome proliferator activated receptors (PPARs) in physiological and pathophysiological processes has been primarily studied in peripherial organs and tissues. Recently it became clear that PPARs play an important role for the pathogenesis of various disorders of the CNS. The finding that activation of PPARs, and in particular, the PPARgamma isoform, suppresses inflammation in peripherial macrophages and in models of human autoimmune disease, instigated the experimental evaluation of these salutary actions for several CNS disorders that have an inflammatory component. Activation of all PPAR isoforms, but especially of PPARgamma, has been found to be protective in murine in vitro and in vivo models of Multiple Sclerosis. The verification of these findings in human cells prompted the initiation of clinical studies evaluating PPARgamma activation in Multiple Sclerosis patients. Likewise, Alzheimer's disease has a prominent inflammatory component that arises in response to neurodegeneration and to extracellular deposition of beta-amyloid peptides. The fact that non steroidal anti-inflammatory drugs (NSAIDs) delay the onset and reduce the risk to develop Alzheimer's disease, while they also bind to and activate PPARgamma, led to the hypothesis that one dimension of NSAID protection in AD may be mediated by PPARgamma. Several lines of evidence from in vitro and in vivo studies have supported this hypothesis, using Alzheimer disease related transgenic cellular and animal models. The ability of PPAR agonists to elicit anti-amyloidogenic, anti-inflammatory and insulin sensitizing effects may account for the observed effects. A number of clinical trials employing PPAR agonists have yielded promising results and further trials are in preparation, which aim to delineate the exact mechanism of interaction. Animal models of other neurodegenerative diseases such as Parkinson's and Amyotrophic lateral sclerosis, both associated with a considerable degree of CNS inflammation, have been studied with a positive outcome. Yet it is not clear whether reduction of inflammation or additional mechanisms account for the observed neuroprotection. Less is known about the physiological role of PPARs for brain development, maintenance and function. Lesions from transgenic mouse models, however, provide evidence that PPARs may play pivotal roles for CNS development and function.
过氧化物酶体增殖物激活受体(PPARs)在生理和病理生理过程中的生物学特性主要是在周围器官和组织中进行研究的。最近发现,PPARs在中枢神经系统各种疾病的发病机制中起着重要作用。PPARs的激活,特别是PPARγ亚型的激活,可抑制外周巨噬细胞和人类自身免疫性疾病模型中的炎症反应,这一发现促使人们对这些有益作用在几种具有炎症成分的中枢神经系统疾病中进行实验评估。已发现所有PPAR亚型的激活,尤其是PPARγ的激活,在小鼠多发性硬化症的体外和体内模型中具有保护作用。在人类细胞中对这些发现的验证促使启动了评估多发性硬化症患者中PPARγ激活情况的临床研究。同样,阿尔茨海默病有一个突出的炎症成分,它是对神经退行性变和β-淀粉样肽的细胞外沉积的反应。非甾体抗炎药(NSAIDs)可延迟阿尔茨海默病的发病并降低其发病风险,同时它们也能结合并激活PPARγ,这一事实导致了这样一种假说,即NSAIDs在阿尔茨海默病中的保护作用的一个方面可能是由PPARγ介导的。来自体外和体内研究的几条证据支持了这一假说,这些研究使用了与阿尔茨海默病相关的转基因细胞和动物模型。PPAR激动剂引发抗淀粉样蛋白生成、抗炎和胰岛素增敏作用的能力可能解释了观察到的效果。一些使用PPAR激动剂的临床试验取得了有希望的结果,并且正在准备进一步的试验,旨在阐明确切机制。其他神经退行性疾病如帕金森病和肌萎缩侧索硬化症的动物模型,这两种疾病都与相当程度的中枢神经系统炎症相关,已进行了研究并取得了阳性结果。然而,尚不清楚炎症的减轻还是其他机制导致了观察到的神经保护作用。关于PPARs在大脑发育、维持和功能方面的生理作用了解较少。然而,转基因小鼠模型的损伤提供了证据表明PPARs可能在中枢神经系统发育和功能中起关键作用。
