Exploring Analysis Approaches for Using the Dopamine Transporter Striatal Binding Ratio in Early- to Mid-Stage Parkinson's Disease Modification Trials.

IF 2.6 4区 医学 Q2 CLINICAL NEUROLOGY
Movement Disorders Clinical Practice Pub Date : 2024-11-01 Epub Date: 2024-08-22 DOI:10.1002/mdc3.14191
Nirosen Vijiaratnam, Christine Girges, Dilan Athauda, Alexa King, Grace Auld, Rachel McComish, Kashfia Chowdhury, Simon Skene, Kate Maclagan, Kallol Ray Chaudhuri, Vincenzo Libri, John Dickson, Thomas Foltynie
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引用次数: 0

Abstract

Background: The dopamine transporter striatal binding ratio (DAT SBR) has been used as an outcome measure in Parkinson's disease (PD) trials of potential disease-modifying therapies; however, both patient characteristics and analysis approach potentially complicate its interpretation.

Objective: The aim was to explore how well DAT SBR reflects PD motor severity across different striatal subregions and the relationship to disease duration, and side of onset.

Methods: DAT SBR for the anterior and posterior putamen and caudate in both hemispheres was obtained using validated automated quantitative software on baseline scans of 132 patients recruited for the Exenatide PD2 and PD3 trials. Associations between mean and lateralized SBR subregions (posterior and anterior putamen and caudate) and summed and lateralized motor characteristics were explored using regression analysis. Analyses were repeated considering disease duration and limiting analysis to the less-affected hemisphere.

Results: Lateralized bradykinesia was most consistently associated with the loss of DAT uptake in the contralateral anterior putamen. There was much higher variance in the posterior putamen, and in all regions in those with longer duration disease, although bradykinesia remained robustly associated with anterior putaminal DAT uptake even in longer-duration patients. Restricting analyses to the less-affected side did not usefully reduce the variance compared to the overall cohort.

Conclusion: These data suggest that DAT SBR could be a useful biomarker in disease-modifying trials, but a focus on anterior striatal subregions and incorporating disease duration into analyses may improve its utility.

探索在帕金森病早中期改良试验中使用多巴胺转运体纹状体结合率的分析方法。
背景:多巴胺转运体纹状体结合率(DAT SBR多巴胺转运体纹状体结合率(DAT SBR)已被用作帕金森病(PD)潜在疾病改变疗法试验的结果测量指标;然而,患者特征和分析方法可能会使其解释复杂化:目的:探讨 DAT SBR 对不同纹状体亚区帕金森病运动严重程度的反映程度,以及与病程和发病侧的关系:方法:在艾塞那肽PD2和PD3试验招募的132名患者的基线扫描中,使用经过验证的自动定量软件获得了两个半球的前部、后部和尾状体的DAT SBR。利用回归分析探讨了平均和侧化 SBR 亚区域(后部和前部普鲁门及尾状核)与总和和侧化运动特征之间的关联。考虑到疾病持续时间,并将分析局限于受影响较小的半球,重复进行了分析:结果:偏侧运动迟缓与对侧前部丘脑的 DAT 摄取丧失关系最为密切。尽管即使在病程较长的患者中,运动迟缓仍与前部丘脑的DAT摄取量密切相关,但在后部丘脑以及病程较长患者的所有区域中,运动迟缓的变异性要高得多。将分析局限于受影响较小的一侧并不能有效减少与整个队列相比的方差:这些数据表明,DAT SBR 可作为疾病改变试验中的一种有用生物标志物,但将重点放在前纹状体亚区并将病程纳入分析可能会提高其效用。
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来源期刊
CiteScore
4.00
自引率
7.50%
发文量
218
期刊介绍: Movement Disorders Clinical Practice- is an online-only journal committed to publishing high quality peer reviewed articles related to clinical aspects of movement disorders which broadly include phenomenology (interesting case/case series/rarities), investigative (for e.g- genetics, imaging), translational (phenotype-genotype or other) and treatment aspects (clinical guidelines, diagnostic and treatment algorithms)
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