Characterizing Parkinson's Disease Clinical and Biomarker Interactions in REM Sleep Behavior Disorder.

medRxiv : the preprint server for health sciences Pub Date : 2025-06-23 DOI:10.1101/2025.05.16.25327469

Vijaya L Reddy, Samantha Esposito, Erika Renkl, Amine Benyakoub, Kara Mead, Camalene Chrysostoum, Sapna Patel, John P Seibyl, Yuan Huang, Brian B Koo, Jesse M Cedarbaum

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Abstract

Background: REM Sleep Behavior Disorder (RBD), marked by dream enactment due to loss of REM-related muscle atonia, is a prominent prodromal indicator of synucleinopathies, particularly Parkinson's Disease (PD).

Objectives: This study aimed to investigate the interplay among key PD biomarkers- α-synuclein seed amplification assay (SAA), hyposmia, and dopamine transporter (DaT) SPECT imaging - in individuals with RBD. Additionally, we evaluated how phenoconversion events and Movement Disorder Society (MDS)-Prodromal PD probability scores relate to clinical symptoms and biomarker profiles in an incident RBD population.

Methods: Participants with polysomnographically-confirmed RBD underwent comprehensive clinical and biomarker assessments. They were grouped along three non-exclusive biomarker-based axes (hyposmic vs. normosmic, SAA positive vs. SAA negative, and DaT positive vs. intermediate vs. negative) and two clinical outcome-based axes (high vs. intermediate/low MDS-Prodromal PD probability; phenoconverters vs. non-phenoconverters). Within each category, performance on various clinical assessments, the presence of other biomarkers, and clinical outcomes were evaluated.

Results: Hyposmia was associated with reductions in striatal DaT binding and α-syn SAA positivity. MDS Prodromal PD Probability Scores, which incorporate DaT and olfactory function, predicted SAA positivity and phenoconversion. DaT positivity was much more common (80%) among phenoconverters (RBD-PC), than non-phenoconverters (10%). No significant motor or non-motor symptom differences were observed between the two groups at baseline, likely due to the small sample size.

Conclusions: α-syn SAA positivity, DaT positivity, and hyposmia are highly associated with each other. MDS Prodromal PD Probability scores may be useful predictors of near-term progression, and thus as stratification factors in clinical research study design.

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表征帕金森病在快速眼动睡眠行为障碍中的临床和生物标志物相互作用。

背景：快速眼动睡眠行为障碍（RBD）是突触核蛋白病，特别是帕金森病（PD）的一个重要前驱指标，其特征是由于快速眼动相关肌肉张力丧失而导致做梦。目的：本研究旨在探讨RBD患者PD关键生物标志物- α-突触核蛋白种子扩增试验（SAA）、低氧和多巴胺转运体（DaT） SPECT成像之间的相互作用。此外，我们评估了表型转化和运动障碍协会(MDS)-前驱PD概率评分与RBD人群临床症状和生物标志物谱的关系。方法：多导睡眠图证实RBD的参与者进行了全面的临床和生物标志物评估。事后，他们按照三个非排他的基于生物标志物的轴（低血症vs正常，SAA阳性vs SAA阴性，DaT阳性vs中间vs阴性）和两个基于临床结果的轴(高vs中/低mds -前驱期PD概率；表型转化者与非表型转化者)。在每个类别中，对各种临床评估的表现、其他生物标志物的存在和临床结果进行了评估。结果：低氧与纹状体多巴胺能活性和α-syn SAA阳性降低密切相关。MDS前驱PD概率评分，结合数据和嗅觉功能，预测SAA阳性和表型转化。在6个表型转换者（RBD-PC）中，DaT阳性比非表型转换者（10%）更常见（80%），但在基线时，两组之间没有观察到显著的运动或非运动症状差异，可能是由于样本量小。结论：α-syn SAA阳性、DaT阳性与低氧血症高度相关。MDS前驱PD概率评分可能是近期进展的有用预测指标，因此可以作为临床研究设计的分层因素。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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medRxiv : the preprint server for health sciences

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