Transcranial Direct Current Stimulation: Effects on Motor and Non-Motor Symptoms of Parkinson’s Disease

Introduction: In the last thirty years, brain neuromodulation techniques have been used as an alternative to pharmacological treatment of neurological disorders. Parkinson’s disease (PD) is a neurodegenerative disorder leading to bradykinesia, rest tremor, postural changes, and non-motor symptoms such as depression, anxiety, sleep disorders, pain, and cognitive decline that compromises executive functions (EFs), responsible for the orderly execution of behaviors and tasks of daily life and intentional and directed actions. To this date, a few studies with transcranial direct current stimulation (tDCS) have shown beneficial effects in PD patients concerning specific motor and non-motor symptoms, targeting the motor cortex and/or prefrontal regions. Objective: The main objective of this study was to evaluate the effects of left prefrontal tDCS across a broad spectrum of motor and non-motor symptoms of PD using established validated scales. Method: Single-blind randomized clinical trial with 18 volunteers with PD, aged between 45 and 80 years (66.1 ± 9.65), who met inclusion and exclusion criteria. Participants were submitted to assessments of motor and non-motor functions employing psychometric scales and tests to evaluate EFs and were randomly divided into two groups: control (sham stimulation) and experimental (active stimulation). All participants were involved in three separate tDCS sessions. The anode was positioned over the left dorsolateral prefrontal cortex and the cathode over the right supraorbital region, with a direct current intensity of 2 mA, lasting 20 minutes. At the end of the three sessions, all participants were reassessed. Results: Significant effects of tDCS on non-motor functions were observed for cognition (verbal fluency of actions, clock copy test, appointment by visual confrontation, and verbal memory with immediate free recall) and subjective assessment of sleep quality (overall restlessness and discomfort in the arms and legs at night, leg and arm cramps at night and distressing dreams). There was also an improvement in the rate of errors and successes for congruent and incongruent stimuli of the Stroop Test. The beneficial effects on motor function were decreased rigidity, improved gait, and greater agility in the finger-tapping test. Conclusion: Three tDCS sessions showed positive results for participants with PD, producing significant improvements in various motor and non-motor functions, including sleep quality, cognition, and EFs. Additionally, the present results indicate that tDCS neuromodulation of the left dorsolateral prefrontal cortex region is feasible, safe, and provides significant objective benefits for PD patients.

Clinical Characteristics of Sleep Disorders in Patients with Parkinson's Disease

In order to investigate the sleep quality and influencing factors in patients with Parkinson＇s disease（PD）, 201 PD patients were enrolled and underwent extensive clinical evaluations. Subjective sleep evaluation was assessed using the Pittsburgh Sleep Quality Index（PSQI）, and the Epworth Sleepiness Scale（ESS）. It was found that poor sleep quality（77.11%） and excessive daytime sleepiness（32.34%） were commonly seen in PD patients and positively correlated with disease severity. Then 70 out of the 201 PD patients and 70 age- and sex-matched controls underwent a polysomnographic recording. The parameters were compared between PD group and control group and the influencing factors of sleep in PD patients were analyzed. The results showed that sleep efficiency（SE） was significantly decreased（P〈0.01）, and sleep latency（SL） and the arousal index（AI） were increased（P〈0.05） in the PD group as compared with those in the control group. SE and total sleep time（TST） were positively correlated with the Hoehn and Yahr（H＆Y） stage. There was significant difference in the extent of hypopnea and hypoxemia between the PD group and the control group（P〈0.05）. Our results indicate that PD patients have an overall poor sleep quality and a high prevalence of sleep disorder, which may be correlated with the disease severity. Respiratory function and oxygen supply are also affected to a certain degree in PD patients.

Sleep Disturbance in Parkinson’s Disease Varies with Age of Onset and Family History

Introduction: Parkinson’s disease (PD) is a progressive neurodegenerative disease more common in those over the age of 60. PD is classically characterized by motor features, although patients may also experience non-motor symptoms. Sleep disturbances, such as rapid eye movement (REM) behavior disorder (RBD), are common in patients with PD and may precede onset of PD. Methods: Data was collected on patients with PD (358 subjects)in a movement disorders clinic at a safety net hospital. In this retrospective database analysis, the association of PD complications with age of onset was evaluated using chi-square tests and logistic regression. Results: Of the PD complications analyzed, there was a significant difference in sleep disturbances by age. Among the 358 PD patients, 120 individuals (33.5%) had information regarding the presence or absence of sleep disturbances. There was a significant difference between the early (onset < 50) and later onset (≥50) groups (p = 0.03) with the odds of having a sleep disorder for the early group 1.6 times that of the late group. Those subjects with siblings who also had PD had 2.0 times the odds of having a sleep disorder compared those without (p = 0.02). Conclusion: Non-motor symptoms such as sleep disorders are a useful predictor of early onset PD. Genetic components of PD impact both motor and non-motor aspects of the disease.

Development of a depression in Parkinson's disease prediction model using machine learning

BACKGROUND It is important to diagnose depression in Parkinson’s disease(DPD)as soon as possible and identify the predictors of depression to improve quality of life in Parkinson’s disease(PD)patients.AIM To develop a model for predicting DPD based on the support vector machine,while considering sociodemographic factors,health habits,Parkinson's symptoms,sleep behavior disorders,and neuropsychiatric indicators as predictors and provide baseline data for identifying DPD.METHODS This study analyzed 223 of 335 patients who were 60 years or older with PD.Depression was measured using the 30 items of the Geriatric Depression Scale,and the explanatory variables included PD-related motor signs,rapid eye movement sleep behavior disorders,and neuropsychological tests.The support vector machine was used to develop a DPD prediction model.RESULTS When the effects of PD motor symptoms were compared using“functional weight”,late motor complications(occurrence of levodopa-induced dyskinesia)were the most influential risk factors for Parkinson's symptoms.CONCLUSION It is necessary to develop customized screening tests that can detect DPD in the early stage and continuously monitor high-risk groups based on the factors related to DPD derived from this predictive model in order to maintain the emotional health of PD patients.

Molecular imaging of movement disorders

Positron emission tomography measures the activity of radioactively labeled compounds which distribute and accumulate in central nervous system regions in proportion to their metabolic rate or blood flow. Specific circuits such as the dopaminergic nigrostriatal projection can be studied with ligands that bind to the pre-synaptic dopamine transporter or post-synaptic dopamine receptors (D1 and D2). Single photon emission computerized tomography (SPECT) measures the activity of similar tracers labeled with heavy radioactive species such as technetium and iodine. In essential tremor, there is cerebellar hypermetabolism and abnormal GABAergic function in premotor cortices, dentate nuclei and ventral thalami, without significant abnormalities in dopaminergic transmission. In Huntington&#x02019;s disease, there is hypometabolism in the striatum, frontal and temporal cortices. Disease progression is accompanied by reduction in striatal D1 and D2 binding that correlates with trinucleotide repeat length, disease duration and severity. In dystonia, there is hypermetabolism in the basal ganglia, supplementary motor areas and cerebellum at rest. Thalamic and cerebellar hypermetabolism is seen during dystonic movements, which can be modulated by globus pallidus deep brain stimulation (DBS). Additionally, GABA-A receptor activity is reduced in motor, premotor and somatosensory cortices. In Tourette&#x02019;s syndrome, there is hypermetabolism in premotor and sensorimotor cortices, as well as hypometabolism in the striatum, thalamus and limbic regions at rest. During tics, multiple areas related to cognitive, sensory and motor functions become hypermetabolic. Also, there is abnormal serotoninergic transmission in prefrontal cortices and bilateral thalami, as well as hyperactivity in the striatal dopaminergic system which can be modulated with thalamic DBS. In Parkinson&#x02019;s disease (PD), there is asymmetric progressive decline in striatal dopaminergic tracer accumulation, which follows a caudal-to-rostral direction. Uptake declines prior to symptom presentation and progresses from contralateral to the most symptomatic side to bilateral, correlating with symptom severity. In progressive supranuclear palsy (PSP) and multiple system atrophy (MSA), striatal activity is symmetrically and diffusely decreased. The caudal-to-rostral pattern is lost in PSP, but could be present in MSA. In corticobasal degeneration (CBD), there is asymmetric, diffuse reduction of striatal activity, contralateral to the most symptomatic side. Additionally, there is hypometabolism in contralateral parieto-occipital and frontal cortices in PD; bilateral putamen and cerebellum in MSA; caudate, thalamus, midbrain, mesial frontal and prefrontal cortices in PSP; and contralateral cortices in CBD. Finally, cardiac sympathetic SPECT signal is decreased in PD. The capacity of molecular imaging to provide in vivo time courses of gene expression, protein synthesis, receptor and transporter binding, could facilitate the development and evaluation of novel medical, surgical and genetic therapies in movement disorders.

Assessing gray matter volume in patients with idiopathic rapid eye movement sleep behavior disorder

Idiopathic rapid eye movement sleep behavior disorder(iRBD) is often a precursor to neurodegenerative disease. However, voxel-based morphological studies evaluating structural abnormalities in the brains of iRBD patients are relatively rare. This study aimed to explore cerebral structural alterations using magnetic resonance imaging and to determine their association with clinical parameters in iRBD patients. Brain structural T1-weighted MRI scans were acquired from 19 polysomnogram-confirmed iRBD patients(male:female 16:3; mean age 66.6 ± 7.0 years) and 20 age-matched healthy controls(male:female 5:15; mean age 63.7 ± 5.9 years). Gray matter volume(GMV) data were analyzed based on Statistical Parametric Mapping 8, using a voxel-based morphometry method and two-sample t-test and multiple regression analysis. Compared with controls, iRBD patients had increased GMV in the middle temporal gyrus and cerebellar posterior lobe, but decreased GMV in the Rolandic operculum, postcentral gyrus, insular lobe, cingulate gyrus, precuneus, rectus gyrus, and superior frontal gyrus. iRBD duration was positively correlated with GMV in the precuneus, cuneus, superior parietal gyrus, postcentral gyrus, posterior cingulate gyrus, hippocampus, lingual gyrus, middle occipital gyrus, middle temporal gyrus, and cerebellum posterior lobe. Furthermore, phasic chin electromyographic activity was positively correlated with GMV in the hippocampus, precuneus, fusiform gyrus, precentral gyrus, superior frontal gyrus, cuneus, inferior parietal lobule, angular gyrus, superior parietal gyrus, paracentral lobule, and cerebellar posterior lobe. There were no significant negative correlations of brain GMV with disease duration or electromyographic activity in iRBD patients. These findings expand the spectrum of known gray matter modifications in iRBD patients and provide evidence of a correlation between brain dysfunction and clinical manifestations in such patients. The protocol was approved by the Ethics Committee of Huashan Hospital(approval No. KY2013-336) on January 6, 2014. This trial was registered in the ISRCTN registry(ISRCTN18238599).

Transcranial sonography in differential diagnosis of Parkinson disease and other movement disorders

Background:Reports evaluating the efficacy of transcranial sonography(TCS)for the differential diagnosis of Parkinson disease(PD)and other movement disorders in China are scarce.Therefore,this study aimed to assess the application of TCS for the differential diagnosis of PD,multiple system atrophy(MSA),progressive supranuclear palsy(PSP),and essential tremor(ET)in Chinese individuals.Methods:From 2017 to 2019,500 inpatients treated at the Department of Dyskinesia,Beijing Tiantan Hospital,Capital Medical University underwent routine transcranial ultrasound examination.The cross-sections at the midbrain and thalamus levels were scanned,and the incidence rates of substantia nigra(SN)positivity and the incidence rates of lenticular hyperechoic area were recorded.The echo of the SN was manually measured.Results:Of the 500 patients,125 were excluded due to poor signal in temporal window sound transmission.Among the 375 individuals with good temporal window sound transmission,200 were diagnosed with PD,90 with ET,50 with MSA,and 35 with PSP.The incidence rates of SN positivity differed significantly among the four patient groups(χ^(2)=121.061,P<0.001).Between-group comparisons were performed,and the PD group showed a higher SN positivity rate than the ET(χ^(2)=94.898,P<0.017),MSA(χ^(2)=57.619,P<0.017),and PSP(χ^(2)=37.687,P<0.017)groups.SN positivity showed a good diagnostic value for differentiating PD from the other three movement diseases,collectively or individually.The incidences of lenticular hyperechoic area significantly differed among the four patient groups(χ^(2)=38.904,P<0.001).Next,between-group comparisons were performed.The lenticular hyperechoic area was higher in the PD group than in the ET(χ^(2)=6.714,P<0.017)and MSA(χ^(2)=18.680,P<0.017)groups but lower than that in the PSP group(χ^(2)=0.679,P>0.017).Conclusion:SN positivity could effectively differentiate PD from ET,PSP,and MSA in a Chinese population.

帕金森病睡眠障碍结构特征及其影响因素的临床研究

目的 探讨帕金森病(PD)患者睡眠障碍的发生率、睡眠结构特征、影响因素。方法 选取2016年8月—2022年4月就诊于河北医科大学第一医院神经内科门诊及住院的101例PD患者为研究对象。应用UPDRS-Ⅲ和H-Y分期对患者运动功能及疾病严重程度进行评价。对PD患者进行PSQI量表、ESS量表、IRLS量表、RBD量表等测试,并测量患者身高、体重、BMI、颈围、腹围、询问既往病史等,所有患者均接受了标准化的夜间多导睡眠监测。结果(1)101例PD患者中有87例(86.14%)存在睡眠障碍。(2)PSG显示PD患者的睡眠障碍常见的有RBD、PLM和OSAHS。(3)PD-RBD患者REM期睡眠比例为(13.14±8.11)%,主观睡眠质量较差且伴有明显的抑郁情绪。(4)PD患者PLM易伴随RLS同时出现。(5)PD-OSAHS在颈围及腹围较大的PD患者中更易发生,与BMI值并无明显相关性,PD-OSAHS患者EDS更常见,对患者日间功能影响更大。结论 PD患者睡眠障碍的患病率较高,PD伴发睡眠障碍患者多表现为RBD、PLM和OSAHS等方面,PD-RBD患者睡眠质量较差且伴有明显的抑郁情绪,PDOSAHS在颈围及腹围较大的PD患者中更易发生,与BMI值并无明显相关性。

基于视频库的翻转课堂在运动障碍疾病教学中的应用

目的探讨基于视频库的翻转课堂在运动障碍疾病教学中的效果。方法建立运动障碍疾病标准化诊断视频库。将2020年6—12月在浙江大学医学院附属第二医院神经内科实习的本科阶段医学生分为对照组和教改组。对照组采用常规教学方法,教改组采用翻转课堂法。课后2组学生进行国际帕金森和运动障碍协会统一帕金森病评分量表第3部分(unified parkinson’s disease rating scale,UPDRS-3)评估,统计与标准分的差距。2组互换教学模式,再次评估MDS-UPDRS-3量表。最后,进行2组间教学满意度的评价比较。结果第一阶段结束,对照组与标准分差值Δ_(A1)为(7.43±2.60)分、教改组与标准分差值Δ_(B1)为(4.90±2.62)分,教改组小于对照组(P<0.05)。第二阶段结束,2组学生评分与标准分差值Δ_(A2)和Δ_(B2)的差异无统计学意义(P>0.05)。教改组的教学满意度高于对照组(P<0.01)。结论与传统的教学方式相比,基于视频学习的翻转课堂可以使学生更快、更好地掌握帕金森病的诊断思路和查体方法。同时在学生满意度方面也有很大的优势,体现了这种方法在运动障碍疾病教学中的良好效果。

以运动障碍专科医生为主导、社区医生为中心的帕金森病管理模式效果研究

背景帕金森病(PD)的发病率逐年增高,增加了医保的疾病负担,目前的慢性病管理模式在PD患者的社区管理中没有发挥作用。目的探讨以运动障碍专科医生为主导、社区医生为中心的PD管理模式的效果,以期提高社区医生的PD综合管理能力,提高PD患者的生活质量。方法选取2022年1月—2023年5月在内蒙古科技大学包头医学院第二附属医院神经内科接受诊治的102例PD患者为研究对象,采用随机数字表法分为对照组和主动干预组各51例。对照组患者接受常规社区管理,主动管理组患者接受以PD为亚专业的社区医生的主动管理,管理内容包括用药调整、运动康复、饮食营养、认知功能障碍和精神功能障碍管理等。分别于患者回归社区的1周内(管理前)和6个月时(管理后)对患者开展评价,评价内容包括单日左旋多巴等效剂量、统一帕金森病评定量表第三部分(UPDRS-Ⅲ)、统一帕金森病评定量表第四部分(UPDRS-Ⅳ)、Hoehn-Yahr(H-Y)分期、39项帕金森病生活质量调查问卷(PDQ-39)。结果管理6个月时,主动管理组患者的左旋多巴等效剂量高于管理前,UPDRS-Ⅲ评分、UPDRS-Ⅳ的其他并发症维度得分、PDQ-39得分低于管理前(P<0.05)。Spearman秩相关分析结果显示,主动管理组患者管理前后的PDQ-39得分差值与其精神健康、屈辱感、认知、社会支持、交流、身体不适维度得分差值呈正相关(rs值为0.651~0.893,P<0.05),与UPDRD-Ⅳ得分差值呈正相关(rs=0.338,P<0.05),而与UPDRS-Ⅲ得分差值不相关(P>0.05)。单因素Logistic回归分析结果显示,与对照组相比,主动管理组患者PDQ-39降低的可能性是对照组患者的11.769倍(95%CI=4.340~31.918,P<0.001)。结论以运动障碍专科医生为主导、社区医生为中心的PD管理模式可以提高患者的生活质量,这为PD社区管理提供了参考。

S100钙结合蛋白β与α突触核蛋白与帕金森病患者抑郁及运动障碍的关系

目的研究帕金森病(PD)患者血清S100钙结合蛋白β(S100β)及α突触核蛋白(α-syn)水平与患者抑郁及运动障碍的关系。方法选择2022年1月至12月聊城市人民医院收治的PD患者194例,根据汉密尔顿抑郁量表评分分为非抑郁组102例(0~13分)及抑郁组92例(≥14分)。运动障碍采用Hoehn-Yahr(H-Y)分级及统一帕金森病评定量表Ⅲ(UPDRS-Ⅲ)进行评分,用多因素logistic回归分析PD患者抑郁的独立危险因素,用Spearman相关性分析血清S100β及α-syn水平与患者抑郁及运动障碍的关系。结果抑郁组体质量指数低于非抑郁组,H-Y分级、UPDRS-Ⅲ评分、S100β、α-syn均高于非抑郁组,差异有统计学意义(P<0.05,P<0.01)。多因素logistic回归分析显示,H-Y分级、UPDRS-Ⅲ评分、S100β、α-syn为PD患者抑郁的独立危险因素(P<0.05)。Spearman相关性分析显示,PD患者S100β水平与H-Y分级、UPDRS-Ⅲ评分呈正相关(r=0.698,P=0.005;r=0.637,P=0.011);α-syn水平与H-Y分级、UPDRS-Ⅲ评分呈正相关(r=0.654,P=0.021;r=0.611,P=0.035)。ROC曲线显示,S100β、α-syn诊断PD患者抑郁的截断值分别为486.65μg/L、3894.27 ng/L,曲线下面积分别为0.889(95%CI:0.812~0.923)、0.761(95%CI:0.714~0.828),S100β曲线下面积显著优于α-syn(P<0.05)。结论PD患者血清S100β、α-syn水平与其抑郁发生及运动功能障碍密切相关。

帕金森病伴睡眠障碍的研究进展

帕金森病(PD)是一种与运动和非运动症状相关的大脑退行性疾病,与环境、遗传、神经系统老化等多种因素有关。近年的调查研究显示,中国PD平均患病年龄60岁,在65岁以上人群中,每10万人约1700名患者。睡眠障碍是PD的非运动症状之一,临床表现包括失眠、白天过度嗜睡、不宁腿综合征、快速眼动期睡眠行为障碍以及睡眠呼吸障碍等多种类型。由于存在个体差异,PD伴睡眠障碍疾病治疗过程中应在医生指导下选择最适合患者个体的药物。本文对PD睡眠障碍发病机制和常用药物治疗方案进行综述,希望能够为今后PD伴睡眠障碍的治疗提供新的思路。

伴和不伴快速眼动睡眠行为障碍帕金森病患者自发脑活动的静息态功能磁共振成像研究

目的快速眼动睡眠行为障碍(rapid eye movement sleep behavior disorder,RBD)是帕金森病(Parkinson's disease,PD)常见的非运动症状且是重要预后因素。本研究通过静息态功能磁共振成像,利用度中心度(degreecentrality,DC)和低频振幅(amplitudes of low-frequency fluctuation,ALFF)分析PD伴RBD和不伴有RBD患者组以及健康对照组三组间DC值和ALFF值,探索PD伴RBD患者脑功能活动特征及RBD特异性脑区,探究RBD发生的病理机制。材料与方法招募20例伴有RBD的PD患者(PD-RBD组)、40例无RBD的PD患者(PD-nonRBD组)和44例年龄性别匹配的健康对照(健康对照组),三组被试均接受磁共振扫描。利用静息态数据计算DC值和ALFF值,探测脑功能特征。结果方差分析结果显示三组间DC值主效应脑区为右侧中央前回、颞上回、小脑、额中回(P<0.05,FDR校正);ALFF值主效应脑区为左侧海马旁回、楔叶、舌回(P<0.05,FDR校正)。进一步分析发现相比于PD-nonRBD组,PD-RBD患者表现为右侧额中回DC值升高(t=4.02;P=0.007,FDR校正);左侧楔前叶DC值降低(t=5.30;P=0.009,FDR校正)。相比于健康对照组,PD-RBD患者表现为左侧额上回、小脑、右侧颞上回、左侧颞中回、额中回的DC值升高(P<0.05,FDR校正);左侧中央前回、颞上回和颞中回的DC值降低(P<0.05,FDR校正);右侧楔叶ALFF值降低(P<0.05,FDR校正)。结论PD-RBD在DC和ALFF上有独特的影像学特征,特别是右侧额中回、左侧楔前叶的功能异常可能与PD患者RBD的发生密切相关。

督脉十三针联合五脏俞加膈俞针刺治疗帕金森病临床研究

目的:观察督脉十三针联合五脏俞加膈俞针刺治疗帕金森病患者运动症状的有效性和安全性。方法:将58例帕金森病患者随机分为对照组和治疗组,对照组28例,治疗组30例。治疗组给予督脉十三针联合五脏俞加膈俞针刺治疗,对照组给予常规针刺治疗方案,每周治疗3次,共治疗8周。分别于治疗前后观察两组患者帕金森病综合评价量表(MDS-UPDRS)、10米步行试验(10MWT)、改良Webster症状评分量表、Hoehn-Yahr(H-Y)分级量表的变化情况,并比较临床疗效。结果:治疗后,两组MDS-UPDRS评分、10MWT、改良Webster症状评分均较治疗前下降(P<0.05),且在MDS-UPDRS评分、10MWT的改善方面,治疗组优于对照组(P<0.05),两组改良Webster症状评分变化比较差异无统计学意义(P>0.05),两组治疗前后H-Y分级组内及组间比较差异均无统计学意义(P>0.05)。结论:督脉十三针联合五脏俞加膈俞针刺治疗可改善帕金森病运动症状,提高患者的生活质量。

帕金森病及相关运动障碍疾病眼球运动障碍的研究进展

帕金森病(PD)是中老年人第二大常见的神经系统变性疾病,以黑质多巴胺神经元变性、缺失为主要病理特点,疾病病程长、致残率高,严重影响着患者的生活质量。PD早期临床表现异质性大,起病隐匿,不易与其他运动障碍疾病相鉴别,造成漏诊误诊。因此,早期筛查识别是PD临床诊疗的关键所在。研究发现,PD及相关运动障碍疾病病程早期可出现眼球运动障碍。本文将对PD及相关运动障碍疾病眼球运动障碍的研究进展进行综述。

重复经颅磁刺激治疗帕金森病伴快速眼动睡眠行为障碍观察

目的探讨重复经颅磁刺激对帕金森病伴快速眼动睡眠行为障碍患者实施治疗的可行性与安全性。方法回顾性分析福州市第二医院2021年3月—2023年3月收治的帕金森病伴快速眼动睡眠行为障碍患者病例资料,查阅并筛选出100例帕金森病伴快速眼动睡眠行为障碍患者完整病例,根据治疗方案分为2组,各50例。参照组采取药物治疗,研究组则在参照组治疗基础上配合重复经颅磁刺激治疗。比较2组治疗效果。结果2组患者治疗后的总睡眠时间(total sleep time,TST)、睡眠效率(sleep efficiency,SE)、快速眼动睡眠时间(rapid eye movement sleep,REMS)比治疗前更高,且研究组治疗后的指标[(360.45±25.68)min、(76.15±5.15)%、(12.85±4.32)min]均高于参照组[(317.85±23.12)min、(68.76±4.31)%、(8.05±1.65)min];而睡眠潜伏期(sleeplatency,SL)、醒觉指数(arousalindex,AI)则要低于治疗前,且研究组治疗后的指标[(17.12±3.45)min、(24.05±2.48)次/h]低于参照组[(24.18±4.36)min、(35.36±3.12)次/h],差异有统计学意义(P<0.05)。治疗后,2组的爱泼沃斯嗜睡量表(Epworth sleeping scale,ESS)评分要低于治疗前,且研究组治疗后评分[(6.01±2.02)分]低于参照组[(8.12±2.05)分],而蒙特利尔认知评估量表(Montreal cognitive assess-ment scale,MoCA)评分、PD睡眠量表(PDsleepscale,PDSS)评分高于治疗前,且研究组治疗后的分数[(25.38±2.76)分、(119.85±11.05)分]明显高出参照组[(22.38±2.13)分、(113.15±10.35)分],差异有统计学意义(P<0.05)。2组不良反应发生率比较,差异无统计学意义(P>0.05)。结论对于帕金森病伴快速眼动睡眠行为障碍采取重复经颅磁刺激治疗,可取得良好治疗效果,对于患者的睡眠障碍改善、认知功能改善有积极作用,且不会增加患者的不良反应发生率,具有较高的安全性。

血清8‑羟基脱氧鸟苷和丙二醛与帕金森病认知功能障碍的相关分析

目的探讨帕金森病患者血清8‑羟基脱氧鸟苷(8‑OHdG)和丙二醛(MDA)水平与认知功能障碍及其严重程度的相关性。方法选择2021年2月至2022年2月徐州医科大学附属医院诊断与治疗的126例帕金森病患者,根据是否合并认知功能障碍分为帕金森病认知功能正常组(PDN组,41例)、帕金森病轻度认知障碍组(PD‑MCI组,47例)、帕金森病痴呆组(PDD组,38例),并选择同期50例健康体检者作为对照组。采用Hoehn‑Yahr分期评估帕金森病患者药物“关”期病情严重程度,统一帕金森病评价量表第三部分(UPDRSⅢ)评估药物“关”期运动功能,蒙特利尔认知评价量表(MoCA)评估安静及药物“开”期认知功能障碍严重程度,并测定帕金森病患者和对照者血清8‑OHdG和MDA水平。采用Pearson相关分析及偏相关分析探讨血清8‑OHdG和MDA水平与帕金森病患者MoCA评分的相关性,单因素和多因素Logistic回归分析筛查帕金森病患者发生认知功能障碍的影响因素,受试者工作特征(ROC)曲线评估血清8‑OHdG和MDA预测帕金森病患者发生认知功能障碍风险的效能。结果相关分析显示,帕金森病患者病程(r=‑0.241,P=0.007)、Hoehn‑Yahr分期(r=‑0.333,P=0.007)、8‑OHdG(r=‑0.310,P=0.000)、MDA(r=‑0.291,P=0.004)与MoCA评分呈负相关关系。Logistic回归分析显示,8‑OHdG(OR=1.335,95%CI:1.137~1.568;P=0.000)和MDA(OR=2.928,95%CI:1.676~5.115;P=0.000)水平升高是帕金森病患者发生认知功能障碍的危险因素。ROC曲线显示,8‑OHdG、MDA及二者联合预测帕金森病患者发生认知功能障碍的曲线下面积分别为0.831(95%CI:0.761~0.902,P=0.000)、0.846(95%CI:0.775~0.916,P=0.000)和0.922(95%CI:0.878~0.966,P=0.000)。结论外周血8‑OHdG和MDA有望成为评估帕金森病患者发生认知功能障碍及其严重程度的血清学标志物。

Effect of Rapid Eye Movement Sleep Behavior Disorder on Obstructive Sleep Apnea Severity and Cognition of Parkinson＇s Disease Patients

Background：Rapid eye movement （REM） sleep behavior disorder （RBD） and obstructive sleep apnea （OSA） are the most common sleep disorders in Parkinson’s disease （PD）. The aim of this study was to identify whether RBD could alleviate OSA severity in PD patients and its effect on cognitive impairment.Methods：From February 2014 to May 2017, we recruited 174 PD patients from the Second Affiliated Hospital of Soochow University, all of whom underwent polysomnography （PSG）. We collected clinical data, PSG results, and compared information between patients with and without RBD or OSA by analysis of covariance. We also investigated the effect of these sleep disorders on cognitive impairment using linear regression.Results：We grouped participants as follows： PD only （n = 53）, PD ＋ OSA （n = 29）, PD ＋ RBD （n = 61）, and PD ＋ RBD ＋ OSA （n = 31）. Minimum oxygen saturation （SaO2） during whole sleep and in REM sleep was higher in PD ＋ RBD ＋ OSA patients than that in PD ＋ OSA patients. PD ＋ RBD patients had worse Mini-Mental Status Examination and Montreal Cognitive Assessment （MoCA） scores than those in the PD group （P 〈 0.001）, especially in visuospatial/executive, attention, and memory functions. The PD ＋ OSA group performed worse than the PD group in the delayed recall domain. After adjusting for age, sex, body mass index, education, disease severity, and other sleep disorders, MoCA was negatively associated with OSA （β = ？0.736, P = 0.043） and RBD （β = ？2.575, P 〈 0.001）. The severity of RBD （tonic/phasic electromyography activity） and OSA （apnea-hypopnea index/oxygen desaturation index/minimum SaO2） were also associated with MoCA. The adjusted β values of RBD-related parameters were higher than that for OSA.Conclusions：We found that RBD alleviated OSA severity; however, RBD and OSA together exacerbated PD cognitive impairment. Further studies are needed to evaluate whether OSA treatment can improve cognition in PD.

Rapid Eye Movement Sleep Behavior Disorder Symptoms Correlate with Domains of Cognitive Impairment in Parkinson＆#39;s Disease

Background： Rapid eye movement （REM） sleep behavior disorder （RBD） may be a risk factor for cognitive impairment in patients with Parkinson＆#39;s disease （PD）.However, little is known regarding the relation between the severity of RBD and the different domains of cognitive impairment.The aim of this study was： （1） to investigate the domains of cognitive impairment in patients with PD and RBD, and （2） to explore risk factors for PD-mild cognitive impairment （PD-MCI） and the relationship between RBD severity and impairment in different cognitive domains in PD.Methods： The participants were grouped as follows： PD without RBD （PD-RBD;n =42）, PD with RBD （PD ＋ RBD;n =32）, idiopathic RBD （iRBD;n =15）, and healthy controls （HCs;n =36）.All participants completed a battery of neuropsychological assessment of attention and working memory, executive function, language, memory, and visuospatial function.The information of basic demographics, diseases and medication history, and motor and nonmotor manifestations was obtained and compared between PD-RBD and PD ＋ RBD groups.Particular attention was paid to the severity of RBD assessed by the RBD Questionnaire-Hong Kong （RBDQ-HK） and the RBD Screening Questionnaire （RBDSQ）, then we further examined associations between the severity of RBD symptoms and cognitive levels via correlation analysis.Results： Compared to PD-RBD subjects, PD ＋ RBD patients were more likely to have olfactory dysfunction and their Epworth Sleepiness Scale scores were higher （P 〈 0.05）.During neuropsychological testing, PD ＋ RBD patients performed worse than PD-RBD patients, including delayed memory function, especially.The MCI rates were 33%, 63%, 33%, and 8% for PD-RBD, PD ＋ RBD, iRBD, and HC groups, respectively.RBD was an important factor for the PD-MCI variance （odds ratio =5.204, P =0.018）.During correlation analysis, higher RBDSQ and RBDQ-HK scores were significantly associated with poorer performance on the Trail Making Test-B （errors） and Auditory Verbal Learning Test （delayed recall） and higher RBD-HK scores were also associated with Rey-Osterrieth complex figure （copy） results.Conclusions： When PD-RBD and PD ＋ RBD patients have equivalent motor symptoms, PD ＋ RBD patients still have more olfactory dysfunction and worse daytime somnolence.RBD is an important risk factor for MCI, including delayed memory.Deficits in executive function, verbal delayed memory, and visuospatial function were consistently associated with more severe RBD symptoms.

第九届国际帕金森病暨运动障碍疾病研讨会/中国卒中学会移动医学上海分会会议纪要

本文简要介绍第九届国际帕金森病暨运动障碍疾病研讨会及中国卒中学会移动医学上海论坛的学术内容。会议在2023年6月8日—10日在上海召开,世界神经病学争议大会会务组核心团队支持,由上海交通大学医学院附属第一人民医院及其嘉定分院主办。王晓平、Amos D Korczyn和赵钢教授担任大会主席,来自巴基斯坦、以色列、美国、希腊和瑞典等国家近10位知名专家通过Zoom视频软件进行会议演讲,就帕金森病、脑血管病、癫痫、偏头痛、肝豆状核变性等罕见病进行了广泛的学术交流,并展开了类似世界神经病学争议大会的热烈讨论和辩论,邀请了多位专业的双语(英语⁃中文)同步翻译,取得了很好的交流效果,吸引了国际上超过30000人次以上的观众和听众来收看和收听。