Three cases with chronic obsessive compulsive disorder report gains in wellbeing and function following rituximab treatment

IF 9.6 1区 医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Maike Gallwitz, Isa Lindqvist, Jan Mulder, Annica J. Rasmusson, Anders Larsson, Evelina Husén, Jesper Borin, Peter J. van der Spek, Nour Sabbagh, Anna Widgren, Jonas Bergquist, Simon Cervenka, Joachim Burman, Janet L. Cunningham
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Abstract

Immunological aetiology is supported for a subgroup with obsessive compulsive disorder (OCD) and conceptualized as autoimmune OCD. The longitudinal clinical course is detailed for three severely ill cases with OCD and indications of immunological involvement with off-label rituximab treatment every six months. All cases showed clear and sustained gains regarding symptom burden and function for over 2.5 years. Brief Psychiatric Rating Scale and Yale-Brown Obsessive-Compulsive Inventory Scale scores decreased 67-100% and 44-92%, respectively. These complex cases, prior to rituximab, had very low functioning and disease duration has been eight, nine and 16 years respectively. All three patients had been unsuccessfully treated with at least two antidepressants or anxiolytics, one neuroleptic and cognitive behavioural therapy. Clinical phenotypes and findings were suggestive of possible autoimmune OCD. Indirect immunohistochemistry detected cerebral spinal fluid (CSF) antibodies in all three cases including a novel anti-neuronal staining pattern against mouse thalamic cells. Exploratory analyses of CSF markers and proteomics identified elevated levels of sCD27 and markers indicative of complement pathway activation when compared to CSF from healthy controls. Multidisciplinary collaboration, advanced clinical investigations and rituximab treatment are feasible in a psychiatric setting. The case histories provide a proof of principle for the newly proposed criteria for autoimmune OCD. The findings suggest that clinical red flags and biological measures may predict rituximab response in chronic treatment-resistant OCD. The report provides orientation that may inform the hypotheses and design of future treatment trials.

Abstract Image

三例慢性强迫症患者报告称,在接受利妥昔单抗治疗后,他们的身心健康和功能都得到了改善
免疫学病因在患有强迫症(OCD)的亚群中得到支持,并被概念化为自身免疫性强迫症。本文详细介绍了三例重症强迫症患者的纵向临床病程,以及每六个月接受一次标签外利妥昔单抗治疗的免疫学受累迹象。所有病例在2.5年多的时间里在症状负担和功能方面都有明显而持续的改善。简明精神病评定量表和耶鲁-布朗强迫症量表评分分别下降了67%-100%和44%-92%。在使用利妥昔单抗之前,这些复杂病例的功能非常低下,病程分别为 8 年、9 年和 16 年。这三名患者都曾接受过至少两种抗抑郁药或抗焦虑药、一种神经安定药和认知行为疗法的治疗,但均未获成功。临床表型和检查结果均提示可能患有自身免疫性强迫症。间接免疫组化在所有三个病例中都检测到了脑脊液(CSF)抗体,包括针对小鼠丘脑细胞的新型抗神经元染色模式。对脑脊液标记物和蛋白质组学的探索性分析发现,与健康对照组的脑脊液相比,sCD27和指示补体途径激活的标记物水平升高。多学科协作、先进的临床研究和利妥昔单抗治疗在精神病学环境中是可行的。这些病例为新提出的自身免疫性强迫症标准提供了原则性证明。研究结果表明,临床红旗和生物学指标可预测利妥昔单抗对慢性耐药强迫症的反应。报告提供的方向可为未来治疗试验的假设和设计提供参考。
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来源期刊
Molecular Psychiatry
Molecular Psychiatry 医学-精神病学
CiteScore
20.50
自引率
4.50%
发文量
459
审稿时长
4-8 weeks
期刊介绍: Molecular Psychiatry focuses on publishing research that aims to uncover the biological mechanisms behind psychiatric disorders and their treatment. The journal emphasizes studies that bridge pre-clinical and clinical research, covering cellular, molecular, integrative, clinical, imaging, and psychopharmacology levels.
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