精神病院自身免疫:明确nmdar抗体脑炎患者的10个特征性精神状态特征

A. Al-Diwani, R. Linighan, C. Perkins, G. Critchlow, B. Lennox, M. Leite, S. Manohar, D. Okai, S. Irani
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Network analysis was used to evaluate connectedness of psychopathologic features and a qualitative synthesis distilled recurrent psychopathologic features. Finally, each time point was compared with operationalised diagnoses using an automated classifier and plotted with corresponding symptom complexes over time. Results All had psychiatric features at onset and were seen first by general practitioners or emergency departments. All received an incorrect initial diagnosis (1 neurological, 4 primary psychiatric). Two patients were referred to mental health services and detained while three were admitted to a general hospital. Psychiatric diagnoses spanned psychotic, mood, and stress categories. None had a personal or family history of serious mental illness or substance misuse. Despite the atypicality all were ascribed to non-specific psycho-social aetiologies. 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引用次数: 1

摘要

目的/目的nmdar抗体脑炎常表现为精神症状。然而,新发精神疾病通常不接受详细的生物医学调查。然而,早期诊断和治疗与改善预后相关。在这里,我们使用详细的精神表型来探索这种免疫定义疾病的精神状态异常的本质。方法对连续5例明确的nmdar抗体脑炎患者、护理人员和临床医生进行前瞻性和回顾性半结构化访谈(均为女性,中位年龄=20岁,范围= 16-30岁,卵巢畸胎瘤4例)。2/5使用神经精神量表养老院版(NPI-NH)进行每周多学科评估。网络分析用于评估精神病理特征的连通性,并对复发性精神病理特征进行定性综合。最后,使用自动分类器将每个时间点与可操作的诊断进行比较,并绘制相应的症状复合物随时间的变化。结果所有患者发病时均有精神病学特征,均由全科医生或急诊科就诊。所有患者均接受了错误的初始诊断(1例神经学,4例原发性精神病学)。两名病人被转介到精神卫生服务机构并被拘留,三名病人被送往一家综合医院。精神病诊断包括精神病、情绪和压力类别。没有人有严重精神疾病或药物滥用的个人或家族病史。尽管非典型性,所有归因于非特异性的心理社会病因。由于精神病理(n=2)或明显癫痫发作或运动障碍(n=3)的发展,在发病后4-28天(中位=21天)首次怀疑自身免疫性脑炎。确定了10个一致报告的特征:睡眠障碍,噩梦,混合不稳定的情绪,困惑,不连贯的重复言语,音乐±视觉幻觉,紧张性相,占有样/药物,分离性混乱和行为退化。复合症状迅速达到高峰(3周内)。高峰负担较大,且跨越多个精神病理领域。总的来说,任何单一的原发疾病都很难描述该综合征;混合性情绪-精神-紧张性精神障碍表现最好。此外,它在发病、峰值和分辨率之间显示出明确的定性和诊断转变。结论nmdar抗体脑炎的精神病理是复杂和动态的,可能导致诊断困难。然而,它在个体之间似乎是刻板的,因此可以推导出敏感特征。与精神病和/或情绪障碍结构的不一致以及与“混合的混合物”的更好近似表明可能存在特异性,但需要与原发性疾病比较者进行类似的研究。由于这种疾病只能通过脑脊液抗体测试来排除,实际意义是精神卫生系统需要将腰椎穿刺作为高风险人群的常规实践的一部分。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
25 On being autoimmune in psychiatric places: 10 characteristic mental state features in patients with definite NMDAR-antibody encephalitis
Objectives/Aims NMDAR-antibody encephalitis frequently presents with psychiatric symptoms. However, new-onset mental illness does not usually receive detailed biomedical investigations. Yet, early diagnosis and treatment correlates with improved outcomes. Here we used detailed psychiatric phenotyping to explore the nature of mental state abnormalities in this immunologically-defined illness. Methods Prospective and retrospective semi-structured interviews with patients, carers, and clinicians in five consecutive cases of definite NMDAR-antibody encephalitis (all female, median age=20 years, range=16–30, ovarian teratoma in 4). Weekly multi-disciplinary assessment using the Neuropsychiatric Inventory Nursing Home version (NPI-NH) in 2/5. Network analysis was used to evaluate connectedness of psychopathologic features and a qualitative synthesis distilled recurrent psychopathologic features. Finally, each time point was compared with operationalised diagnoses using an automated classifier and plotted with corresponding symptom complexes over time. Results All had psychiatric features at onset and were seen first by general practitioners or emergency departments. All received an incorrect initial diagnosis (1 neurological, 4 primary psychiatric). Two patients were referred to mental health services and detained while three were admitted to a general hospital. Psychiatric diagnoses spanned psychotic, mood, and stress categories. None had a personal or family history of serious mental illness or substance misuse. Despite the atypicality all were ascribed to non-specific psycho-social aetiologies. Autoimmune encephalitis was then first suspected between 4–28 days from onset (median=21 days) because of the psychopathology (n=2) or development of clear-cut seizures or movement disorder (n=3). 10 consistently reported features were identified: sleep disturbance, nightmares, mixed unstable mood, perplexity, incoherent repetitive speech, musical ±visual hallucinosis, catatonic facies, possession-like/drugged, dissociative-disorganised, and regressed behaviour. The symptom complex peaked rapidly (within 3 weeks). The peak burden was large and crossed multiple psychopathologic domains. Overall the syndrome is poorly-described by any single primary disorder; mixtures of mixed mood-psychotic-catatonic disorders performed best. Furthermore, it showed clear qualitative and hence diagnostic shifts between onset, peak, and resolution. Conclusions The psychopathology of NMDAR-antibody encephalitis is complex and dynamic, likely contributing to diagnostic difficulties. However, it appears stereotyped between individuals, hence sensitive features can be derived. Inconsistency with psychosis and/or mood disorder constructs and better approximation with ‘mixtures of mixtures’ suggests specificity is possible but similar studies with primary disorder comparators are needed. As the disease can only be ruled out with cerebrospinal fluid antibody testing the practical implication is that the mental health system needs to embrace lumbar puncture as a routine part of practice in high risk groups.
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