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首页> 外文期刊>Neurology: Official Journal of the American Academy of Neurology >Age and time course of long-term motor and nonmotor complications in Parkinson disease
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Age and time course of long-term motor and nonmotor complications in Parkinson disease

机译:年龄和时间的长期运动nonmotor帕金森病的并发症

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Objective To determine the time course of hazard for motor and nonmotor milestones of Parkinson disease (PD) in the long term and to investigate whether risk scales nonlinearly with time is instrumental in identifying changes in pathological processes and evaluating disease-modifying therapies in PD. Methods Outpatients with PD at the Lyon University Movement Disorders Center were evaluated for 7 clinical milestones in this retrospective cohort study, encompassing 4 domains of PD progression: (1) motor (motor fluctuations, dyskinesias); (2) axial (postural instability and falls, freezing of gait); (3) neuropsychiatric (impulse control disorders, hallucinations); and (4) cognitive (dementia) complications. For each complication, we estimated the outcome-specific hazard using parsimonious smooth parametric Poisson regression models allowing for nonlinear scaling over disease duration, age at diagnosis, current age, and their interaction. Results A total of 1,232 patients with PD experienced 1,527 disease-related complications in up to 12 years of follow-up. Specific to each complication, hazard rates increased dramatically starting from diagnosis and were highest for motor fluctuations and lowest for dementia up to 6 years after diagnosis in patients aged 65 years at diagnosis. Nonlinear patterns indicated dramatic changes in the course of PD after 5 years and predicted more severe axial prognosis after 70 years and for motor fluctuations, dyskinesias, and impulse control disorders before 60 years at diagnosis. Conclusion Time course of motor and nonmotor milestones in PD is determined by disease duration and age at diagnosis in nonlinear patterns and their interaction. This indicates disease- and age-specific thresholds across the multiple neurodegenerative processes accumulating in PD at different paces.
机译:摘要目的确定风险的时间进程电动机和nonmotor帕金森的里程碑长期疾病(PD)和调查是否与时间是非线性风险在确定的变化病理过程和评估疾病修饰治疗PD。与PD里昂大学门诊病人运动障碍中心进行评估7临床回顾性队列的里程碑研究中,包括4 PD进展的领域:(1)电动机(电机波动、运动困难);轴向(姿势不稳定和下降,冻结步态);失调、幻觉);(老年痴呆症)的并发症。我们估计outcome-specific风险吝啬的光滑参数泊松回归模型允许非线性缩放在诊断疾病持续时间、年龄、当前时代和他们的相互作用。PD患者经历了1527年12年来疾病相关的并发症随访。风险利率急剧增加从诊断和最高运动波动并为痴呆后6年最低65岁的病人在诊断诊断。非线性模式表示戏剧性的变化5年后PD和预测严重的轴向70年和后预后电机波动、动作障碍和冲动控制疾病在诊断前60年。结论时间运动和nonmotor里程碑在PD是由疾病持续时间和年龄在非线性诊断模式和他们的相互作用。疾病和特定的阈值多个神经退化进程积累在PD以不同的速度。

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