阿尔茨海默病患者的视觉结构保留和抗神经自身抗体:一项病例对照研究

Niels Hansen, S. Hirschel, B. Teegen, J. Wiltfang, B. Malchow
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摘要

背景阿尔茨海默病(AD)很少报道与神经自身抗体有关,除了在先前的研究中涉及轴突神经变性和淀粉样变性。然而,这是阿尔茨海默病研究不足的一个方面。由于我们不知道额外筛查AD患者自身抗体是否具有额外的诊断和治疗价值,本研究旨在阐明视觉建构性或图形记忆能力是否可以区分这些患者群体。方法:在这个试点病例系列中,我们研究了8例与脑脊液(CSF)为基础的阿尔茨海默病(AP)相关的认知障碍患者,并验证了抗神经自身抗体(AP Aab+)与8例无自身抗体(Aab -)的AD患者(AD Aab -)。通过CERAD(建立阿尔茨海默病登记联盟)测试组和AMDP(精神病学精神病理学评估和记录手册)系统对患者档案进行回顾性回顾,以评估他们的神经心理特征。我们还依赖脑脊液和磁共振图像的诊断参数。结果所有患者都有类似海马体依赖性记忆功能障碍的单词表学习和单词表回忆功能障碍模式。此外,两组患者的脑脊液特征都与阿尔茨海默病一致。然而,AP Aab阳性患者的视觉建构能力,而不是图形回忆能力,而AD ab -患者的共同海马基础记忆功能障碍则没有。我们观察到在脑脊液细胞计数或鞘内IgG合成方面,AP Aab+组和AD Aab -组之间没有相关差异。AP Aab+组和AD Aab -组海马和局灶性萎缩的相对频率也无差异。我们的初步研究结果鼓励我们进行大规模的研究,以复制我们在AP Aab阳性的海马记忆功能障碍患者中保留的视觉结构的发现。抗神经自身抗体的作用仍未完全了解。这些自身抗体的检测可能暗示另一种疾病病理,可能是神经保护或影响其他大脑区域,即在主要涉及视觉构建的右侧颞顶叶区域不太明显的疾病活动。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Preserved visuoconstruction in patients with Alzheimer's pathology and anti-neural autoantibodies: A case control study
Background Alzheimer's disease (AD) is seldom reported to be associated with neural autoantibodies apart from those involved in axonal neurodegeneration and amyloidopathy in prior studies. Nevertheless, this is an under-investigated aspect of AD. As we do not know whether additional screening for autoantibodies in AD patients has additional diagnostic and therapeutic value, this study aims to shed light on whether visuoconstructive or figural memory capacities might distinguish these patient populations. Methods In this pilot case series, we investigated eight patients suffering from cognitive impairment associated with cerebrospinal fluid (CSF)-based Alzheimer pathology (AP) and with verified anti-neural autoantibodies (AP Aab+) compared to eight AD patients presenting no autoantibodies (Aab–) (AD Aab–). Patients files were reviewed retrospectively regarding their neuropsychological profile assessed via the CERAD (Consortium to Establish a Registry for Alzheimer's Disease) test battery and psychopathology measured by the AMDP (Manual for the Assessment and Documentation of Psychopathology in Psychiatry) system. We also relied on diagnostic parameters as in the CSF and magnetic resonance images. Results All patients shared the same pattern of dysfunctional word-list learning and word-list recall resembling a hippocampus-dependent memory dysfunction. Furthermore, both patient groups revealed a CSF profile concurring with Alzheimer's disease. However, visuoconstructive capacity, but not figure recall was preserved in AP Aab+ patients, but not in AD Ab-patients with the shared hippocampus-based memory dysfunction. We observed no relevant differences between the AP Aab+ and AD Aab– groups in CSF cell-counts or intrathecal IgG synthesis. The relative frequency of hippocampal and focal atrophy did not differ either between AP Aab+ and AD Aab– groups. Discussion Our pilot findings are encouraging us to conduct large-scale studies to replicate our discovery of preserved visuoconstruction in AP Aab+ patients with hippocampus-based memory dysfunction. The role of anti-neural autoantibodies is still not fully understood. The detection of these autoantibodies might imply another disease pathology that could be either neuroprotective or be affecting other brain regions, i.e., less pronounced disease activity in the right temporo-parietal regions mainly involved in visuoconstruction.
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