纹状体结合率的下降与帕金森病精神病患者符号数字模型(Symbol Digit Modality)表现的加速下降有关,但与 MoCA 无关

Sara Pisani, Latha Velayudhan, Dag Aarsland, K Ray Chaudhuri, Clive Ballard, Dominic ffytche, Sagnik Bhattacharyya
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摘要

背景:帕金森病精神病(PDP)中有认知缺陷的报道。多巴胺转运体(DAT)结合率降低也与帕金森病有关。然而,DAT纹状体结合率(SBR)是否会导致帕金森病患者认知能力的恶化,目前仍不清楚。在此,我们利用帕金森病进展标志物倡议研究的数据对此进行了研究:我们分析了 408 名帕金森病患者从基线到第 4 年随访期间的数据,并将患者分为帕金森病伴精神病(PDP)和不伴精神病(PDnP)两类。DAT SBR可通过123 I-FP-CIT-SPECT的DaTSCAN成像获得。我们检查了在每个时间点评估的所有认知指标,并将社会人口统计学、神经精神疾病和帕金森病特异性症状作为相关协变量进行了输入。结果与帕金森综合症患者相比,帕金森综合症患者的 DAT SBR 更低(b=-0.092,p=0.035),在控制了年龄、性别和种族因素后,这一结果仍然显著。与 PDnP 患者相比,PDP 患者四年来在 MoCA(b=-0.238,p=0.001)和符号数字模型(b=-0.534,p=0.016)方面的任务表现轨迹也较差。PDP患者MoCA评分的恶化与DAT SBR的下降无关(交互作用组*研究年限,b=-0.284,p=0.016;三方交互作用组*研究年限*DAT SBR,b=0.127,p=0.225)。然而,符号数字模型成绩的下降与DAT SBR的下降显著相关(三向交互组*学习年限*DAT SBR,b=0.683,p=0.028):总之,纹状体突触前多巴胺功能的纵向下降可能是导致PD精神病患者在涉及处理速度、联想学习和工作记忆的符号数字模态任务中成绩纵向下降幅度较大的原因,而MoCA成绩的下降似乎与此无关。纹状体突触前多巴胺的变化是否能解释帕金森病患者在其他认知领域加速纵向衰退的原因还有待检验。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Decline in striatal binding ratio associated with accelerated decline in performance on Symbol Digit Modality but not MoCA in Parkinson's disease psychosis
Background: Cognitive deficits have been reported in Parkinson's Disease psychosis (PDP). Reduced dopamine transporter (DAT) binding ratio has also been associated with PDP. However, it remains unclear whether DAT striatal binding ratio (SBR) may contribute to worsening cognitive performance in PDP. Here, we examined this using data from the Parkinson's Progression Markers Initiative study. Methods: We analysed data from 408 PD patients, from baseline to year 4 follow up, and classified patients into PD with (PDP) and without psychosis (PDnP). DAT SBR was available from DaTSCAN imaging with 123 I-FP-CIT-SPECT. We examined all cognitive measures assessed at each time point, socio-demographics, neuropsychiatric and PD-specific symptoms were entered as covariates of interest. Results: PDP patients had lower DAT SBR compared to PDnP patients (b=-0.092, p=0.035) which remained significant after controlling for age, sex, and ethnicity. PDP patients also reported worse trajectory of task performance on MoCA (b=-0.238, p=0.001) and Symbol Digit Modality (b=-0.534, p=0.016) across four years compared to PDnP patients. Worsening of MoCA scores in PDP was independent of DAT SBR decline (interaction group * study years, b=-0.284, p=0.016; three-way interaction group*study years*DAT SBR, b=0.127, p=0.225). However, declining performance in Symbol Digit Modality was significantly associated with the decline in DAT SBR (three-way interaction group*study years*DAT SBR, b=0.683, p=0.028). Conclusion: Overall, longitudinal decline in striatal presynaptic dopamine function may underlie the greater longitudinal decline in performance in the symbol digit modality task that engages processing speed, associative learning and working memory in PD psychosis, whilst declining performance on MoCA seems unrelated to it. Whether striatal presynaptic dopamine changes explain accelerated longitudinal decline in other cognitive domains in people with PDP remains to be tested.
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