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帕金森病药物反应的神经生理学预测指标

Neurophysiological Predictors of Response to Medication in Parkinson's Disease.

作者信息

Filipović Saša R, Kačar Aleksandra, Milanović Sladjan, Ljubisavljević Miloš R

机构信息

Department for Human Neuroscience, Institute for Medical Research, University of Belgrade, Belgrade, Serbia.

Department of Neurology, Faculty of Medicine, University of Belgrade, Belgrade, Serbia.

出版信息

Front Neurol. 2021 Nov 16;12:763911. doi: 10.3389/fneur.2021.763911. eCollection 2021.

Abstract

Although dopaminergic medication has been the foundation of Parkinson's disease (PD) therapy for decades, sensitive and specific therapeutic response biomarkers that allow for better treatment optimization are lacking. We tested whether the features of Transcranial Magnetic Stimulation-based neurophysiological measures taken off-medication are associated with dopaminergic medication-induced clinical effects. Motor cortex excitability [short-latency intracortical inhibition (SICI), intracortical facilitation (ICF), short-latency afferent inhibition (SAI), and input-output (IO) curve], and plasticity [paired associative stimulation (PAS) protocol] neurophysiological measures were examined in 23 PD patients off-medication. Clinical features were quantified by the motor section of the Unified Parkinson's Disease Scale (total score and lateralized total, bradykinesia, and rigidity sub-scores), and the differences between measures off-medication and on-medication (following the usual morning dose), were determined. Total daily dopaminergic medication dose (expressed as levodopa equivalent daily dose-LEDD), was also determined. SICI significantly correlated with changes in lateralized UPDRS motor and bradykinesia sub-scores, suggesting that patients with stronger basal intracortical inhibition benefit more from dopaminergic treatment than patients with weaker intracortical inhibition. Also, ICF significantly negatively correlated with LEDD, suggesting that patients with stronger intracortical facilitation require less dopaminergic medication to achieve optimal therapeutic benefit. Both associations were independent of disease severity and duration. The results suggest variability of (patho) physiological phenotypes related to intracortical inhibitory and facilitatory mechanisms determining clinical response to dopaminergic medication in PD. Measures of intracortical excitability may help predict patients' response to dopaminergic therapy, thus potentially providing a background for developing personalized therapy in PD.

摘要

尽管几十年来多巴胺能药物一直是帕金森病(PD)治疗的基础,但仍缺乏能够实现更好治疗优化的敏感且特异的治疗反应生物标志物。我们测试了停药时基于经颅磁刺激的神经生理学测量特征是否与多巴胺能药物诱导的临床效果相关。对23名停药的PD患者进行了运动皮层兴奋性[短潜伏期皮层内抑制(SICI)、皮层内易化(ICF)、短潜伏期传入抑制(SAI)和输入-输出(IO)曲线]以及可塑性[配对联想刺激(PAS)方案]的神经生理学测量。通过统一帕金森病评定量表的运动部分(总分以及单侧总分、运动迟缓及强直子评分)对临床特征进行量化,并确定停药和服药时(按照常规早晨剂量)测量值之间的差异。还确定了每日多巴胺能药物总剂量(以左旋多巴等效日剂量-LEDD表示)。SICI与单侧UPDRS运动和运动迟缓子评分的变化显著相关,这表明基础皮层内抑制较强的患者比皮层内抑制较弱的患者从多巴胺能治疗中获益更多。此外,ICF与LEDD显著负相关,这表明皮层内易化较强的患者达到最佳治疗效果所需的多巴胺能药物较少。这两种关联均独立于疾病严重程度和病程。结果表明,与皮层内抑制和易化机制相关的(病理)生理表型存在变异性,这些机制决定了PD患者对多巴胺能药物的临床反应。皮层内兴奋性测量可能有助于预测患者对多巴胺能治疗的反应,从而有可能为PD个性化治疗的发展提供依据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/47ca/8635106/a30a3b036c5d/fneur-12-763911-g0001.jpg

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