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什么因素可预测帕金森病患者的死亡率?一项基于人群的前瞻性长期研究。

What predicts mortality in Parkinson disease?: a prospective population-based long-term study.

机构信息

The Norwegian Center for Movement Disorders, Stavanger University Hospital, Box 8100, N-4068 Stavanger, Norway.

出版信息

Neurology. 2010 Oct 5;75(14):1270-6. doi: 10.1212/WNL.0b013e3181f61311.

Abstract

OBJECTIVE

To identify independent risk factors of mortality in a community-based Parkinson disease (PD) cohort during prospective long-term follow-up.

METHODS

A community-based prevalent sample of 230 patients with PD from southwestern Norway was followed prospectively with repetitive assessments of motor and nonmotor symptoms from 1993 to 2005. Information on vital status until October 20, 2009, was obtained from the National Population Register in Norway. Cox proportional hazards models were applied to identify independent predictors of mortality during follow-up. Chronological age, Unified Parkinson's Disease Rating Scale (UPDRS) motor score, levodopa equivalent dose, probable REM sleep behavior disorder, psychotic symptoms, dementia, and use of antipsychotics were included as time-dependent variables, and age at onset (AAO) and sex as time-independent variables.

RESULTS

Of 230 patients, 211 (92%) died during the study period. Median survival time from motor onset was 15.8 years (range 2.2-36.6). Independent predictors of mortality during follow-up were AAO (hazard ratio [HR] 1.40 for 10-years increase, p = 0.029), chronological age (HR 1.51 for 10-years increase, p = 0.043), male sex (HR 1.63, p = 0.001), UPDRS motor score (HR 1.18 for 10-point increase, p < 0.001), psychotic symptoms (HR 1.45, p = 0.039), and dementia (HR 1.89, p = 0.001).

CONCLUSIONS

This population-based long-term study demonstrates that in addition to AAO, chronological age, motor severity, and dementia, psychotic symptoms independently predict increased mortality in PD. In contrast, no significant impact of antipsychotic or antiparkinsonian drugs on survival was observed in our PD cohort. Early prevention of motor progression and development of psychosis and dementia may be the most promising strategies to increase life expectancy in PD.

摘要

目的

在一项社区帕金森病(PD)队列的前瞻性长期随访中,确定死亡率的独立危险因素。

方法

对来自挪威西南部的 230 名社区确诊 PD 患者进行了一项基于社区的前瞻性研究,从 1993 年到 2005 年,对运动和非运动症状进行了反复评估。截至 2009 年 10 月 20 日,通过挪威国家人口登记处获取了患者的生存状态信息。采用 Cox 比例风险模型来确定随访期间死亡率的独立预测因素。将年龄、统一帕金森病评定量表(UPDRS)运动评分、左旋多巴等效剂量、可能的 REM 睡眠行为障碍、精神病症状、痴呆和抗精神病药物的使用作为时间依赖性变量,发病年龄(AAO)和性别作为时间独立性变量。

结果

230 例患者中,211 例(92%)在研究期间死亡。从运动发病到中位生存时间为 15.8 年(范围 2.2-36.6)。随访期间死亡率的独立预测因素包括 AAO(每增加 10 年,风险比 [HR] 为 1.40,p = 0.029)、年龄(每增加 10 年,HR 为 1.51,p = 0.043)、男性(HR 为 1.63,p = 0.001)、UPDRS 运动评分(每增加 10 分,HR 为 1.18,p < 0.001)、精神病症状(HR 为 1.45,p = 0.039)和痴呆(HR 为 1.89,p = 0.001)。

结论

这项基于人群的长期研究表明,除了 AAO 外,年龄、运动严重程度和痴呆症外,精神病症状也可独立预测 PD 患者的死亡率增加。相反,我们的 PD 队列中未观察到抗精神病药物或抗帕金森药物对生存率有显著影响。早期预防运动进展和精神病和痴呆的发生可能是提高 PD 患者预期寿命的最有前途的策略。

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