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针对铁代谢失衡的神经退行性疾病治疗策略。

Targeting Iron Dyshomeostasis for Treatment of Neurodegenerative Disorders.

机构信息

Buffalo Neuroimaging Analysis Center, Department of Neurology, Jacobs School of Medicine and Biomedical Sciences, University at Buffalo, State University of New York, 100 High St., Buffalo, NY, 14203, USA.

Center for Biomedical Imaging, Clinical and Translational Science Institute, University at Buffalo, State University of New York, Buffalo, NY, USA.

出版信息

CNS Drugs. 2019 Nov;33(11):1073-1086. doi: 10.1007/s40263-019-00668-6.

Abstract

While iron has an important role in the normal functioning of the brain owing to its involvement in several physiological processes, dyshomeostasis has been found in many neurodegenerative disorders, as evidenced by both histopathological and imaging studies. Although the exact causes have remained elusive, the fact that altered iron levels have been found in disparate diseases suggests that iron may contribute to their development and/or progression. As such, the processes involved in iron dyshomeostasis may represent novel therapeutic targets. There are, however, many questions about the exact interplay between neurodegeneration and altered iron homeostasis. Some insight can be gained by considering the parallels with respect to what occurs in healthy aging, which is also characterized by increased iron throughout many regions in the brain along with progressive neurodegeneration. Nevertheless, the exact mechanisms of iron-mediated damage are likely disease specific to a certain degree, given that iron plays a crucial role in many disparate biological processes, which are not always affected in the same way across different neurodegenerative disorders. Moreover, it is not even entirely clear yet whether iron actually has a causative role in all of the diseases where altered iron levels have been noted. For example, there is strong evidence of iron dyshomeostasis leading to neurodegeneration in Parkinson's disease, but there is still some question as to whether changes in iron levels are merely an epiphenomenon in multiple sclerosis. Recent advances in neuroimaging now offer the possibility to detect and monitor iron levels in vivo, which allows for an improved understanding of both the temporal and spatial dynamics of iron changes and associated neurodegeneration compared to post-mortem studies. In this regard, iron-based imaging will likely play an important role in the development of therapeutic approaches aimed at addressing altered iron dynamics in neurodegenerative diseases. Currently, the bulk of such therapies have focused on chelating excess iron. Although there is some evidence that these treatment options may yield some benefit, they are not without their own limitations. They are generally effective at reducing brain iron levels, as assessed by imaging, but clinical benefits are more modest. New drugs that specifically target iron-related pathological processes may offer the possibility to prevent, or at the least, slow down irreversible neurodegeneration, which represents an unmet therapeutic target.

摘要

虽然铁在许多神经退行性疾病中通过参与几个生理过程对大脑的正常功能起着重要作用,但在组织病理学和影像学研究中都发现了铁动态平衡失调。虽然确切的原因仍未可知,但在不同疾病中发现改变的铁水平这一事实表明,铁可能有助于这些疾病的发展和/或进展。因此,涉及铁动态平衡失调的过程可能代表新的治疗靶点。然而,关于神经退行性变和铁动态平衡改变之间的确切相互作用仍存在许多问题。通过考虑与健康衰老相关的相似之处,可以获得一些见解,健康衰老也表现为大脑许多区域的铁含量增加,同时进行性神经退行性变。然而,由于铁在许多不同的生物学过程中起着至关重要的作用,并且这些过程在不同的神经退行性疾病中并不总是以相同的方式受到影响,因此铁介导的损伤的确切机制在某种程度上可能是疾病特异性的。此外,甚至还不完全清楚铁是否实际上在所有观察到铁水平改变的疾病中都具有因果作用。例如,在帕金森病中,铁动态平衡失调导致神经退行性变的证据很强,但铁水平的变化是否仅仅是多发性硬化症中的一个偶然现象仍存在一些疑问。神经影像学的最新进展现在提供了在体内检测和监测铁水平的可能性,这使得与死后研究相比,可以更好地理解铁变化和相关神经退行性变的时间和空间动态。在这方面,基于铁的成像可能在开发针对神经退行性疾病中改变的铁动态的治疗方法中发挥重要作用。目前,此类治疗的大部分方法都集中在螯合多余的铁上。尽管有一些证据表明这些治疗选择可能会带来一些益处,但它们并非没有自己的局限性。它们通常在通过成像评估时有效降低大脑铁水平,但临床益处则更为适度。专门针对与铁相关的病理过程的新药可能有希望预防或至少减缓不可逆转的神经退行性变,这是一个未满足的治疗靶点。

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