EARLY RECOGNITION OF COGNITIVE ABILITY AND NUTRITIONAL MARKERS FOR DEMENTIA IN PARKINSON’S DISEASE

JAR life Pub Date : 2018-01-01 DOI:10.14283/jarcp.2018.26
L. Håglin, L. Bâckman, J. Linder, L. Forsgren, M. Domellöf
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Abstract

Background: Cognitive decline and dementia are common non-motor problems in Parkinson’s disease (PD). The underlying aetiology is multifaceted and both chronic and reversible causes for cognitive decline are likely to be present. Malnutrition is frequent in the Parkinson population, both early and late in the disease, and nutritional deficiencies could play a role in some cognitive deficits. Objectives: The objective is to study the association between nutritional status with focus on iron intake and homeostasis, mild cognitive impairment (MCI), and PD dementia (PDD). Setting and Participants: This study included 73 out of 145 patients with PD participating in a population-based study in northern Sweden. Measurements: Registration of nutritional status by laboratory analyses of blood plasma and neuropsychological assessments at time of diagnosis were performed. MCI and PDD were assessed yearly up to ten years after diagnosis. Mini Nutritional Assessments (Full-MNA score) and plasma variables detecting iron homeostasis were compared between patients with MCI and patients with normal cognition (NC). Motor severity was measured using the Unified Parkinson´s disease rating scale III, (UPDRS III) and Hoehn and Yahr (H&Y) staging scale. Cox proportional Hazard model were performed to see if any variables that differed between MCI and NC could predict PDD at follow-up. Results: Patients with MCI at time of diagnosis had lower levels of plasma iron (P-Fe) and albumin (P-Albumin) as well as a lower score on Full-MNA score. Dietary intake of iron was higher in patients with MCI than in patients with NC (p = 0.012). In logistic regression models adjusted for age, sex, and UPDRS III, lower levels of P-Fe (p = 0.025) and P-Albumin (p = 0.011) and higher dietary iron intake (p = 0.019) were associated with MCI at baseline. A Cox regression model with dementia as endpoint revealed that lower levels of P-Fe increase the risk of dementia at follow-up with adjustments for age, sex, UPDRS III, and MCI at baseline (HR 95% CI = 0.87 (0.78-0.98), p = 0.021). Conclusions: Low P-Fe was associated with cognitive disturbance at baseline and predicted dementia up to ten years after diagnosis in patients with PD. Low P-Albumin and malnutrition assessed with Full-MNA score were associated with MCI at baseline but did not predict dementia at follow-up.
帕金森病患者认知能力和营养指标的早期识别
背景:认知能力下降和痴呆是帕金森病(PD)常见的非运动问题。潜在的病因是多方面的,认知能力下降的慢性和可逆原因都可能存在。营养不良在帕金森患者中很常见,无论是在疾病的早期还是晚期,营养缺乏可能在一些认知缺陷中起作用。目的:目的是研究营养状况(关注铁摄入和体内平衡)、轻度认知障碍(MCI)和PD痴呆(PDD)之间的关系。环境和参与者:本研究纳入了145名PD患者中的73名,这些患者参加了瑞典北部的一项基于人群的研究。测量方法:诊断时通过血浆实验室分析和神经心理学评估登记营养状况。MCI和PDD在诊断后10年内每年进行一次评估。比较MCI患者和认知正常患者(NC)的Mini营养评估(Full-MNA评分)和血浆铁稳态检测变量。运动严重程度采用统一帕金森病评定量表III (UPDRS III)和Hoehn and Yahr (H&Y)分期量表进行测量。采用Cox比例风险模型,观察MCI和NC之间是否存在差异的变量可以预测随访时的PDD。结果:诊断时MCI患者血浆铁(P-Fe)和白蛋白(P-Albumin)水平较低,Full-MNA评分较低。MCI患者的膳食铁摄入量高于NC患者(p = 0.012)。在调整了年龄、性别和UPDRS III的logistic回归模型中,较低水平的p - fe (p = 0.025)和p -白蛋白(p = 0.011)以及较高的膳食铁摄入量(p = 0.019)与基线时的MCI相关。以痴呆为终点的Cox回归模型显示,在调整年龄、性别、UPDRS III和基线时MCI后,较低水平的p - fe增加了痴呆的风险(HR 95% CI = 0.87 (0.78-0.98), p = 0.021)。结论:低P-Fe与基线认知障碍有关,并预测PD患者诊断后10年内的痴呆。以Full-MNA评分评估的低p -白蛋白和营养不良与基线时的MCI相关,但不能预测随访时的痴呆。
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