Non-motor asymmetry and dopamine degeneration in Parkinson's disease.

IF 4.5 Q1 CLINICAL NEUROLOGY Brain communications Pub Date : 2025-01-06 eCollection Date: 2025-01-01 DOI:10.1093/braincomms/fcaf002
Frederik O Hansen, Karoline Knudsen, Malene F Damholdt, Toke Bek, Per Borghammer, Niels Okkels
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Abstract

Asymmetric dopaminergic degeneration of the striatum is a characteristic feature of Parkinson's disease, associated with right-left asymmetry in motor function. As such, studying asymmetry provides insights into progressive neurodegeneration between cerebral hemispheres. Given the impact of Lewy pathology on various neurotransmitter systems beyond the dopaminergic, it may be that other neuronal systems in the predominantly affected hemisphere are similarly affected. According to this hypothesis, asymmetry in dopaminergic degeneration would be expected to coincide with asymmetry in other neurotransmitter systems. Consequently, asymmetry in functions primarily dependent on dopaminergic integrity, such as motor function, should correlate with asymmetry in bilateral non-motor functions that rely on other cerebral systems, such as pupillary function. Therefore, this study tested whether right-left asymmetry in bilateral non-motor measures correlates with asymmetry in dopaminergic striatal integrity. We also tested whether asymmetric striatal degeneration is associated with greater asymmetry in non-motor measures overall. Using a comparative cross-sectional design, we recruited newly diagnosed patients with Parkinson's disease with predominantly right-sided (n = 18), left-sided (n = 15) or symmetric nigrostriatal denervation (n = 15) assessed on dopamine PET. Detailed examinations of lateralized non-motor function included lacrimation, hand skin wrinkling, salivation, olfaction and pupillary function. Healthy controls were recruited for comparison. We observed a moderate-to-strong correlation between right-left asymmetry of putamen dopamine binding and asymmetry in pupillary redilation speed [Spearman's rank correlation coefficient (rs ) = -0.53, 95% confidence interval (-0.77; -0.14), P = 0.0084]. We also observed moderate correlations between non-negative putaminal asymmetry and lacrimation [rs = 0.35, (-0.00; 0.62), P = 0.0464] and word recognition [rs = 0.36, (0.01; 0.63), P = 0.0410]. However, none were significant after false discovery rate correction. We observed significant group differences in non-negative asymmetry in salivation (P = 0.0390, ANOVA) and a trend towards greater asymmetric lacrimation in participants with asymmetric striatal dopamine loss compared with healthy controls (P = 0.0330, unadjusted). Additionally, participants with asymmetric striatal dopaminergic binding showed greater, though non-significant, asymmetry in all pupillary measures compared with those with symmetric dopaminergic binding. In conclusion, this study contributes to our understanding of neurodegeneration progression in Parkinson's disease and suggests a link between dopaminergic degeneration and non-motor measures related to autonomic function, particularly salivation, lacrimation and pupillary function. While our findings do not support a strict right-left hemispheric association between non-motor functions and dopaminergic degeneration, potential relationships may exist between these features and asymmetrical degeneration in other neuronal systems, such as the cholinergic.

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帕金森病的非运动不对称和多巴胺变性。
纹状体的不对称多巴胺能变性是帕金森病的一个特征,与运动功能的左右不对称有关。因此,研究不对称提供了对大脑半球之间进行性神经变性的见解。考虑到Lewy病理对多巴胺能以外的各种神经递质系统的影响,可能主要受影响半球的其他神经系统也受到类似影响。根据这一假设,多巴胺能变性的不对称性与其他神经递质系统的不对称性是一致的。因此,主要依赖于多巴胺能完整性的功能的不对称性,如运动功能,应该与依赖于其他大脑系统的双侧非运动功能的不对称性相关,如瞳孔功能。因此,本研究测试了双侧非运动测量的左右不对称是否与多巴胺能纹状体完整性的不对称相关。我们还测试了非对称纹状体变性是否与总体非运动测量中更大的不对称有关。采用比较横断面设计,我们招募了以多巴胺PET评估为主的右侧(n = 18)、左侧(n = 15)或对称黑质纹状体失神经(n = 15)的新诊断帕金森病患者。侧化非运动功能的详细检查包括流泪、手部皮肤起皱、唾液分泌、嗅觉和瞳孔功能。招募健康对照进行比较。我们观察到壳核多巴胺结合的左右不对称性与瞳孔再扩张速度的不对称性之间存在中等到强的相关性[Spearman等级相关系数(rs) = -0.53, 95%可信区间(-0.77;-0.14), p = 0.0084]。我们还观察到非负性壳层不对称与流泪有中等相关性[rs = 0.35, (-0.00;0.62), P = 0.0464]和单词识别[rs = 0.36, (0.01;0.63), p = 0.0410]。然而,在错误发现率校正后,没有显著性差异。我们观察到,与健康对照组相比,不对称纹状体多巴胺丢失的参与者在非负性不对称唾液分泌方面存在显著的组间差异(P = 0.0390,方差分析),不对称流泪的趋势更大(P = 0.0330,未经校正)。此外,纹状体多巴胺能结合不对称的参与者与对称多巴胺能结合的参与者相比,在所有瞳孔测量中表现出更大的不对称,尽管不显著。总之,本研究有助于我们理解帕金森病的神经变性进展,并提示多巴胺能变性与自主神经功能相关的非运动测量之间存在联系,特别是唾液分泌、流泪和瞳孔功能。虽然我们的研究结果不支持左右半球非运动功能和多巴胺能变性之间的严格联系,但这些特征与其他神经系统(如胆碱能)的不对称变性之间可能存在潜在的关系。
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审稿时长
6 weeks
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Motor neuron disease can present as a paraneoplastic neurologic syndrome with various phenotypes. Examining neuroimaging biomarkers, plasma biomarkers and cognitive functions in patients with recovered COVID-19 infection: a multicentre study using 7T MRI. Passing the torch at Brain Communications. Brain-injury and Alzheimer's disease biomarkers are elevated in patients with suspected infection and physiological derangement: importance for context-specific interpretation of Alzheimer's biomarkers. Hippocampal morphometry is altered in infants with congenital heart disease.
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