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帕金森病中脑相关网络退变的纵向三模态成像

Longitudinal trimodal imaging of midbrain-associated network degeneration in Parkinson's disease.

作者信息

Steidel Kenan, Ruppert Marina C, Greuel Andrea, Tahmasian Masoud, Maier Franziska, Hammes Jochen, van Eimeren Thilo, Timmermann Lars, Tittgemeyer Marc, Drzezga Alexander, Pedrosa David J, Eggers Carsten

机构信息

Department of Neurology, University Hospital of Marburg, Marburg, Germany.

Center for Mind, Brain and Behavior-CMBB, Universities Marburg and Gießen, Marburg, Germany.

出版信息

NPJ Parkinsons Dis. 2022 Jun 22;8(1):79. doi: 10.1038/s41531-022-00341-8.

Abstract

The prevailing network perspective of Parkinson's disease (PD) emerges not least from the ascending neuropathology traceable in histological studies. However, whether longitudinal in vivo correlates of network degeneration in PD can be observed remains unresolved. Here, we applied a trimodal imaging protocol combining 18F-fluorodeoxyglucose (FDG)- and 18F-fluoro-L-Dopa- (FDOPA)-PET with resting-state functional MRI to assess longitudinal changes in midbrain metabolism, striatal dopamine depletion and striatocortical dysconnectivity in 17 well-characterized PD patients. Whole-brain (un)paired-t-tests with focus on midbrain or striatum were performed between visits and in relation to 14 healthy controls (HC) in PET modalities. Resulting clusters of FDOPA-PET comparisons provided volumes for seed-based functional connectivity (FC) analyses between visits and in relation to HC. FDG metabolism in the left midbrain decreased compared to baseline along with caudatal FDOPA-uptake. This caudate cluster exhibited a longitudinal FC decrease to sensorimotor and frontal areas. Compared to healthy subjects, dopamine-depleted putamina indicated stronger decline in striatocortical FC at follow-up with respect to baseline. Increasing nigrostriatal deficits and striatocortical decoupling were associated with deterioration in motor scores between visits in repeated-measures correlations. In summary, our results demonstrate the feasibility of in-vivo tracking of progressive network degeneration using a multimodal imaging approach. Specifically, our data suggest advancing striatal and widespread striatocortical dysfunction via an anterior-posterior gradient originating from a hypometabolic midbrain cluster within a well-characterized and only mild to moderately affected PD cohort during a relatively short period.

摘要

帕金森病(PD)目前流行的网络观点至少部分源于组织学研究中可追溯的上行神经病理学。然而,PD 网络退化的纵向体内相关性是否能够被观察到仍未得到解决。在此,我们应用了一种三模态成像方案,将 18F-氟脱氧葡萄糖(FDG)和 18F-氟-L-多巴(FDOPA)正电子发射断层扫描(PET)与静息态功能磁共振成像相结合,以评估 17 例特征明确的 PD 患者中脑代谢、纹状体多巴胺耗竭和纹状体 - 皮质失连接的纵向变化。在 PET 模态下,在各次就诊之间以及与 14 名健康对照(HC)进行比较时,进行了以中脑或纹状体为重点的全脑(非)配对 t 检验。FDOPA-PET 比较得出的聚类为各次就诊之间以及与 HC 相关的基于种子点的功能连接(FC)分析提供了体积数据。与基线相比,左侧中脑的 FDG 代谢减少,同时尾状核的 FDOPA 摄取也减少。这个尾状核聚类在与感觉运动和额叶区域的纵向 FC 上有所下降。与健康受试者相比,在随访时,多巴胺耗竭的壳核相对于基线显示出纹状体 - 皮质 FC 更强的下降。在重复测量相关性中,黑质纹状体缺陷增加和纹状体 - 皮质解耦与各次就诊之间运动评分的恶化相关。总之,我们的结果证明了使用多模态成像方法在体内追踪进行性网络退化的可行性。具体而言,我们的数据表明,在一个特征明确且仅轻度至中度受影响的 PD 队列中,在相对较短的时间内,通过源自低代谢中脑聚类的前后梯度,纹状体和广泛的纹状体 - 皮质功能障碍在不断进展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/32df/9218128/b9ac9d8c06d8/41531_2022_341_Fig1_HTML.jpg

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