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首页> 外文期刊>Journal of neuroinflammation >Mapping neuroinflammation in frontotemporal dementia with molecular PET imaging
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Mapping neuroinflammation in frontotemporal dementia with molecular PET imaging

机译:利用分子PET成像定位额颞叶痴呆的神经炎症

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Recent findings have led to a renewed interest and support for an active role of inflammation in neurodegenerative dementias and related neurologic disorders. Detection of neuroinflammation in vivo throughout the course of neurodegenerative diseases is of great clinical interest. Studies have shown that microglia activation (an indicator of neuroinflammation) may present at early stages of frontotemporal dementia (FTD), but the role of neuroinflammation in the pathogenesis of FTD is largely unknown. The first-generation translocator protein (TSPO) ligand ([11C]-PK11195) has been used to detect microglia activation in FTD, and the second-generation TSPO ligands have imaged neuroinflammation in vivo with improved pharmacokinetic properties. This paper reviews related literature and technical issues on mapping neuroinflammation in FTD with positron-emission tomography (PET) imaging. Early detection of neuroinflammation in FTD may identify new tools for diagnosis, novel treatment targets, and means to monitor therapeutic efficacy. More studies are needed to image and track neuroinflammation in FTD. It is anticipated that the advances of TSPO PET imaging will overcome technical difficulties, and molecular imaging of neuroinflammation will aid in the characterization of neuroinflammation in FTD. Such knowledge has the potential to shed light on the poorly understood pathogenesis of FTD and related dementias, and provide imaging markers to guide the development and assessment of new therapies.
机译:最近的发现引起了人们对炎症在神经退行性痴呆和相关神经系统疾病中的积极作用的新的兴趣和支持。在整个神经退行性疾病的过程中体内神经炎症的检测具有重大的临床意义。研究表明,小胶质细胞活化(神经炎症的指标)可能在额颞叶痴呆(FTD)的早期出现,但是神经炎症在FTD发病机理中的作用尚不清楚。第一代转运蛋白(TSPO)配体([11C] -PK11195)已用于检测FTD中的小胶质细胞活化,第二代TSPO配体对体内的神经炎症成像,具有改善的药代动力学特性。本文回顾了有关正电子发射断层扫描(PET)成像在FTD中绘制神经炎症的相关文献和技术问题。 FTD中神经炎症的早期发现可能会确定新的诊断工具,新的治疗目标以及监测治疗效果的手段。需要更多的研究来成像和跟踪FTD中的神经炎症。可以预期,TSPO PET成像技术的发展将克服技术难题,而神经炎症的分子成像技术将有助于FTD中神经炎症的表征。这些知识有可能阐明人们对FTD和相关痴呆的知之甚少的发病机理,并提供成像标记以指导新疗法的开发和评估。

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