精神病性路易体痴呆前驱期的临床表现和拟议生物标记物的诊断应用。

Ryota Kobayashi, Kuniyuki Iwata-Endo, Hiroshige Fujishiro
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引用次数: 0

摘要

路易体痴呆(DLB)前驱期诊断的研究标准包括三种临床亚型:路易体轻度认知障碍(MCI-LB)、谵妄前驱期DLB和精神病前驱期DLB。晚期精神症状表现者患痴呆症的风险较高,但其与前驱型DLB的关系仍不清楚。除了严重的抗精神病药物超敏反应风险外,由于管理和预后方面的潜在差异,准确区分非 DLB 病例也很重要。本文旨在回顾这一迅速发展的精神科话题,并概述精神科前驱 DLB 的临床表现,包括 MCI-LB 的生物标志物发现:多导睡眠图证实的快速眼动睡眠行为障碍、心脏[123I]偏二苄基胍闪烁成像和纹状体多巴胺转运体成像。我们首先回顾了尸检证实的 DLB 患者的临床图片。在临床报告方面,我们重点关注了主要表现为精神症状,随后发展为 DLB 的患者。随后,我们回顾了有关晚期精神病患者诊断应用拟议生物标志物的临床研究。临床表现主要是晚发性抑郁症和精神病,但也有其他临床表现的报道。在确诊 DLB 之前服用精神药物可能会导致锥体外系症状,并有可能影响所提出的生物标记物的发现。在治疗精神症状的过程中,这些风险会使临床表现的解释复杂化。需要进行纵向随访研究,在转为 DLB 之前进行标准化评估,以研究核心特征的时间轨迹和拟议的生物标志物结果。在晚发性精神障碍患者中,对精神疾病前驱 DLB 患者的识别为更好地了解具有发生痴呆症高风险的独特预后亚群提供了机会。在建立用于检测病理α-突触核蛋白的直接生物标记物方面取得的进展,可能会促进前驱DLB表型变异的重组。
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Clinical presentations and diagnostic application of proposed biomarkers in psychiatric-onset prodromal dementia with Lewy bodies.

Research criteria for the diagnosis of prodromal dementia with Lewy bodies (DLB) include three clinical subtypes: mild cognitive impairment with Lewy bodies (MCI-LB), delirium-onset prodromal DLB, and psychiatric-onset prodromal DLB. Late-onset psychiatric manifestations are at a higher risk of developing dementia, but its relation to prodromal DLB remains unclear. In addition to the risk of severe antipsychotic hypersensitivity reactions, accurate discrimination from non-DLB cases is important due to the potential differences in management and prognosis. This article aims to review a rapidly evolving psychiatric topic and outline clinical pictures of psychiatric-onset prodromal DLB, including the proposed biomarker findings of MCI-LB: polysomnography-confirmed rapid eye movement sleep behaviour disorder, cardiac [123I]metaiodobenzylguanidine scintigraphy, and striatal dopamine transporter imaging. We first reviewed clinical pictures of patients with autopsy-confirmed DLB. Regarding clinical reports, we focused on the patients who predominantly presented with psychiatric manifestations and subsequently developed DLB. Thereafter, we reviewed clinical studies regarding the diagnostic applications of the proposed biomarkers to patients with late-onset psychiatric disorders. Clinical presentations were mainly late-onset depression and psychosis; however, other clinical manifestations were also reported. Psychotropic medications before a DLB diagnosis may cause extrapyramidal signs, and potentially influences the proposed biomarker findings. These risks complicate clinical manifestation interpretation during the management of psychiatric symptoms. Longitudinal follow-up studies with standardised evaluations until conversion to DLB are needed to investigate the temporal trajectories of core features and proposed biomarker findings. In patients with late-onset psychiatric disorders, identification of patients with psychiatric-onset prodromal DLB provides the opportunity to better understanding the distinct prognostic subgroup that is at great risk of incident dementia. Advances in the establishment of direct biomarkers for the detection of pathological α-synuclein may encourage reorganising the phenotypic variability of prodromal DLB.

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