Räty Valtteri, Kuusimäki Tomi, Majuri Joonas, Vahlberg Tero, Gardberg Maria, Noponen Tommi, Seppänen Marko, Tolppanen Anna-Maija, Kaasinen Valtteri
Clinical Neurosciences, University of Turku, Finland.
Neurocenter, Turku University Hospital, Finland.
Neurology. 2025 May 13;104(9):e213499. doi: 10.1212/WNL.0000000000213499. Epub 2025 Apr 4.
Accurate diagnosis of Parkinson disease (PD) remains challenging, with variability and clinical uncertainty, especially in nonspecialized settings. Despite advancements in diagnostic criteria and biological markers, misdiagnosis continues to affect patient care and research. This study aimed to assess the long-term diagnostic stability of PD and evaluate the accuracy of initial diagnoses over time in a large, consecutive cohort diagnosed by neurologists, with or without movement disorder specialization.
We conducted a retrospective longitudinal analysis of patients diagnosed with PD between 2006 and 2020. Patient records were reviewed over a median follow-up period of 10 years, with more than half of the cohort tracked from motor symptom onset to death. Diagnostic evaluations included dopamine transporter (DAT) imaging and neuropathologic examinations for a subset of patients, based on clinical indications. Two movement disorder specialists cross-validated diagnoses through retrospective chart reviews.
The cohort included 1,626 patients (mean age 69.0 years, 44.1% female). Of these, 10.6% (n = 172) had their diagnoses revised by treating neurologists, and 2.7% (n = 44) were revised based on chart reviews or neuropathologic findings. The median time to diagnosis revision was 22 months (interquartile range = 43). The most common revised diagnoses were vascular parkinsonism, progressive supranuclear palsy, and multiple system atrophy, with 4.7% (n = 77) classified as clinically undetermined parkinsonism. In a secondary analysis separating PD and dementia with Lewy bodies (DLB), the revision rate increased to 17.7%. DAT imaging had been performed on 588 patients and was more frequently used in revised cases. Postmortem neuropathologic examinations had been conducted in only 3% of deceased patients, with 64% confirming the initial PD diagnosis.
This study demonstrates significant diagnostic instability in PD, with 13.3% of diagnoses revised, primarily within 2 years. When DLB is considered separately, the revision rate increases to 17.7%. Despite frequent DAT imaging and limited postmortem examinations, clinical uncertainty persists among practicing neurologists, contrasting with lower misdiagnosis rates in specialized centers. These findings highlight the need for systematic application of diagnostic criteria, regular reevaluation of diagnoses, more frequent autopsies, and the development of accessible diagnostic biomarkers.
帕金森病(PD)的准确诊断仍然具有挑战性,存在变异性和临床不确定性,尤其是在非专科环境中。尽管诊断标准和生物标志物有所进展,但误诊仍继续影响患者护理和研究。本研究旨在评估PD的长期诊断稳定性,并评估在由神经科医生诊断的大型连续队列中,无论是否具有运动障碍专科背景,随着时间推移初始诊断的准确性。
我们对2006年至2020年间诊断为PD的患者进行了回顾性纵向分析。在中位随访期10年期间对患者记录进行了审查,超过一半的队列从运动症状出现追踪至死亡。根据临床指征,对一部分患者进行了多巴胺转运体(DAT)成像和神经病理学检查。两名运动障碍专科医生通过回顾性病历审查对诊断进行了交叉验证。
该队列包括1626名患者(平均年龄69.0岁,44.1%为女性)。其中,10.6%(n = 172)的患者诊断被治疗神经科医生修订,2.7%(n = 44)根据病历审查或神经病理学发现进行了修订。诊断修订的中位时间为22个月(四分位间距 = 43)。最常见的修订诊断为血管性帕金森综合征、进行性核上性麻痹和多系统萎缩,4.7%(n = 77)被归类为临床未定型帕金森综合征。在将PD与路易体痴呆(DLB)分开的二次分析中,修订率增至17.7%。对588名患者进行了DAT成像,且在修订病例中使用更频繁。仅3%的已故患者进行了尸检神经病理学检查,64%的检查结果证实了初始PD诊断。
本研究表明PD存在显著的诊断不稳定性,13.3%的诊断被修订,主要在2年内。当单独考虑DLB时,修订率增至17.7%。尽管频繁进行DAT成像且尸检检查有限,但执业神经科医生中临床不确定性仍然存在,这与专科中心较低的误诊率形成对比。这些发现凸显了系统应用诊断标准、定期重新评估诊断、更频繁进行尸检以及开发可及的诊断生物标志物的必要性。
