Department of Psychiatry, University of Magdeburg, Magdeburg, Germany.
JAMA Psychiatry. 2013 Mar;70(3):271-8. doi: 10.1001/2013.jamapsychiatry.86.
Evidence for symptomatic convergence of schizophrenia and N-methyl-D-aspartate glutamate receptor (NMDA-R) encephalitis highlights the need for an assessment of antibody prevalence and specificity for distinct disease mechanisms in patients with a diagnosis of schizophrenia among glutamatergic pathophysiologic abnormalities in psychiatric disorders.
To compare the specificity and prevalence of NMDA-R antibodies in schizophrenia (DSM-IV criteria) with those of other psychiatric diagnoses and to determine whether antibody subtypes characterize overlap with and distinction from those in NMDA-R encephalitis.
Serum from 459 patients admitted with acute schizophrenia, major depression (MD), and borderline personality disorder (BLPD) or individuals serving as matched controls was obtained from our scientific blood bank. To explore epitope specificity and antibody subtype, IgA/IgG/IgM NMDA-R (NR1a or NR1a/NR2b) and α-amino-3-hydroxyl-5-methyl-4-isoxazole-propionate receptors (AMPA-R) (GluR1/GluR2) serum antibodies were determined.
Two hundred thirty matched healthy controls were compared with patients (unmedicated for at least 6 weeks) with schizophrenia (n = 121), MD (n = 70), or BLPD (n = 38).
The primary outcome was the overall number of seropositive cases for NMDA-R and AMPA-R antibodies; the secondary outcome was disease specificity of IgA/IgG/IgM antibodies and epitope specificity for clinical subgroups.
Diverse NMDA-R antibodies were identified in 15 subjects, primarily those with an initial schizophrenia diagnosis (9.9%), opposed to MD (2.8%), BLPD (0), and controls (0.4%). Retrospectively, 2 patients initially classified as having catatonic or disorganized schizophrenia were reclassified as having misdiagnosed NMDA-R encephalitis (presence of specific serum and cerebrospinal fluid IgG NR1a antibodies). In all other seropositive cases, the antibodies consisted of classes IgA and/or IgM or were directed against NR1a/NR2b (not against NR1a alone). None of the patients or controls had antibodies against AMPA-R.
Acutely ill patients with an initial schizophrenia diagnosis show an increased prevalence of NMDA-R antibodies. The repertoire of antibody subtypes in schizophrenia and MD is different from that with NMDA-R encephalitis. The latter disorder should be considered as a differential diagnosis, particularly in young females with acute disorganized behavior or catatonia.
精神分裂症和 N-甲基-D-天冬氨酸谷氨酸受体(NMDA-R)脑炎的症状趋同证据强调了需要评估抗体在精神障碍谷氨酸能病理生理异常中的患病率和对特定疾病机制的特异性,以用于诊断为精神分裂症的患者。
比较精神分裂症(DSM-IV 标准)患者 NMDA-R 抗体的特异性和患病率与其他精神诊断的特异性和患病率,并确定抗体亚型是否能区分和重叠 NMDA-R 脑炎。
从我们的科学血库获得了 459 名因急性精神分裂症、重性抑郁症(MD)和边缘性人格障碍(BLPD)入院或作为匹配对照的个体的血清。为了探索表位特异性和抗体亚型,测定了 IgA/IgG/IgM NMDA-R(NR1a 或 NR1a/NR2b)和α-氨基-3-羟基-5-甲基-4-异恶唑丙酸受体(AMPA-R)(GluR1/GluR2)血清抗体。
将 230 名匹配的健康对照与未经治疗至少 6 周的精神分裂症(n=121)、MD(n=70)或 BLPD(n=38)患者进行比较。
主要结局是 NMDA-R 和 AMPA-R 抗体的总阳性病例数;次要结局是 IgA/IgG/IgM 抗体的疾病特异性和临床亚组的表位特异性。
在 15 名患者中鉴定出多种 NMDA-R 抗体,主要是那些最初诊断为精神分裂症的患者(9.9%),而 MD(2.8%)、BLPD(0)和对照(0.4%)。回顾性地,2 名最初归类为有紧张型或瓦解型精神分裂症的患者被重新归类为误诊的 NMDA-R 脑炎(存在特异性血清和脑脊液 IgG NR1a 抗体)。在所有其他阳性抗体的病例中,抗体由 IgA 和/或 IgM 组成,或针对 NR1a/NR2b(而非仅针对 NR1a)。没有患者或对照者有抗 AMPA-R 抗体。
最初诊断为精神分裂症的急性病患者 NMDA-R 抗体的患病率增加。精神分裂症和 MD 中的抗体亚型谱与 NMDA-R 脑炎不同。后者应被视为鉴别诊断,特别是在有急性瓦解性行为或紧张症的年轻女性中。
