神经元α-突触核蛋白病综合分期系统在 PPMI、PASADENA 和 SPARK 基线队列中的表现

IF 6.7 1区 医学 Q1 NEUROSCIENCES
Tien Dam, Gennaro Pagano, Michael C. Brumm, Caroline Gochanour, Kathleen L. Poston, Daniel Weintraub, Lana M. Chahine, Christopher Coffey, Caroline M. Tanner, Catherine M. Kopil, Yuge Xiao, Sohini Chowdhury, Luis Concha-Marambio, Peter DiBiaso, Tatiana Foroud, Mark Frasier, Danna Jennings, Karl Kieburtz, Kalpana Merchant, Brit Mollenhauer, Thomas J. Montine, Kelly Nudelman, John Seibyl, Todd Sherer, Andrew Singleton, Diane Stephenson, Matthew Stern, Claudio Soto, Eduardo Tolosa, Andrew Siderowf, Billy Dunn, Tanya Simuni, Kenneth Marek
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引用次数: 0

摘要

神经元α-突触核蛋白病(NSD)的生物学定义和综合分期系统(NSD-ISS)提供了一个研究框架,用于识别路易体病理学患者,并根据潜在的生物学特征和功能障碍的程度对他们进行分期。利用来自 PPMI、PASADENA 和 SPARK 研究的数据,我们为 NSD-ISS 开发并应用了跨疾病连续体的生物和临床数据定义。根据基线时的生物、临床和功能锚,我们将入选者定义为帕金森病患者、前驱期患者或健康对照者,并对其进行分期。三项研究中共有 1741 名参与者获得了 SAA 数据,其中 1030 人(59%)的 S+ 与 NSD 一致。在散发性帕金森病患者中,683/736(93%)人属于NSD,2B、3和4期的分布比例分别为25%、63%和9%。基线 2B、3 和 4 期出现有临床意义结果的中位时间(95% CI)分别为 8.3(6.2,10.1)年、5.9(4.1,6.0)年和 2.4(1.0,4.0)年。我们为 NSD-ISS 提出了试验性的生物和临床锚点。我们的研究结果突显了目前被定义为早期帕金森病患者的基线异质性。基线阶段可预测进展到具有临床意义的里程碑的时间。有必要在纵向队列中进一步研究验证这些锚点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Neuronal alpha-Synuclein Disease integrated staging system performance in PPMI, PASADENA, and SPARK baseline cohorts

Neuronal alpha-Synuclein Disease integrated staging system performance in PPMI, PASADENA, and SPARK baseline cohorts

The Neuronal alpha-Synuclein Disease (NSD) biological definition and Integrated Staging System (NSD-ISS) provide a research framework to identify individuals with Lewy body pathology and stage them based on underlying biology and increasing degree of functional impairment. Utilizing data from the PPMI, PASADENA, and SPARK studies, we developed and applied biologic and clinical data-informed definitions for the NSD-ISS across the disease continuum. Individuals enrolled as Parkinson’s disease, Prodromal, or Healthy Controls were defined and staged based on biological, clinical, and functional anchors at baseline. Across the three studies 1741 participants had SAA data and of these 1030 (59%) were S+ consistent with NSD. Among sporadic PD, 683/736 (93%) were NSD, and the distribution for Stages 2B, 3, and 4 was 25%, 63%, and 9%, respectively. Median (95% CI) time to developing a clinically meaningful outcome was 8.3 (6.2, 10.1), 5.9 (4.1, 6.0), and 2.4 (1.0, 4.0) years for baseline stage 2B, 3, and 4, respectively. We propose pilot biologic and clinical anchors for NSD-ISS. Our results highlight the baseline heterogeneity of individuals currently defined as early PD. Baseline stage predicts time to progression to clinically meaningful milestones. Further research on validation of the anchors in longitudinal cohorts is necessary.

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来源期刊
NPJ Parkinson's Disease
NPJ Parkinson's Disease Medicine-Neurology (clinical)
CiteScore
9.80
自引率
5.70%
发文量
156
审稿时长
11 weeks
期刊介绍: npj Parkinson's Disease is a comprehensive open access journal that covers a wide range of research areas related to Parkinson's disease. It publishes original studies in basic science, translational research, and clinical investigations. The journal is dedicated to advancing our understanding of Parkinson's disease by exploring various aspects such as anatomy, etiology, genetics, cellular and molecular physiology, neurophysiology, epidemiology, and therapeutic development. By providing free and immediate access to the scientific and Parkinson's disease community, npj Parkinson's Disease promotes collaboration and knowledge sharing among researchers and healthcare professionals.
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