Psychiatrists are increasingly involved in the diagnosis and management of patients with autoimmune encephalitis, and many patients present initially to psychiatrists. The commonest cause of autoimmune encephalitis in children and young people is N-methyl-d-aspartate receptor (NMDAR) antibody encephalitis (NMDARE), in which antibodies against the GluN1 subunit of NMDAR cause a severe and progressive neuropsychiatric syndrome characterised in the later stages by encephalopathy, seizures and movement disorder, but frequently presenting in the early stages with prominent psychiatric or behavioural symptoms that can be difficult to differentiate from primary psychiatric disease.Reference Dalmau, Armangué, Planagumà, Radosevic, Mannara and Leypoldt1
The psychopathological features of NMDARE are well characterised in adults,Reference Al-Diwani, Handel, Townsend, Pollak, Leite and Harrison2 but less understood in children and adolescents, despite over a third of cases occurring in this group.Reference Titulaer, McCracken, Gabilondo, Armangué, Glaser and Iizuka3 Diagnosis of autoimmune encephalitis in patients presenting with psychiatric symptoms is often delayed;Reference Herken and Pruss4 as earlier treatment is associated with a better outcome in both children and adultsReference Titulaer, McCracken, Gabilondo, Armangué, Glaser and Iizuka3,Reference Byrne, Walsh, Hacohen, Muscal, Jankovic and Stocco5 recognition of psychiatric features in children is clearly important. Catatonia is frequently reported in adults with NMDARE but has never been systematically evaluated in children with the disease.Reference Herken and Pruss4,Reference Espinola-Nadurille, Flores-Rivera, Rivas-Alonso, Vargas-Cañas, Fricchione and Bayliss6,Reference Rogers, Pollak, Blackman and David7 We therefore analysed individually reported paediatric patients with NMDARE to assess the prevalence and symptomatology of catatonia and the relationship to clinical characteristics and outcome.
Method
We previously reported a MEDLINE literature search for first-episode cases of paediatric NMDARE, identifying individually reported data in 80 children (≤17 years) across 34 publications (see Byrne et al Appendix e-1).Reference Byrne, Walsh, Hacohen, Muscal, Jankovic and Stocco5 Only cases of patients with adequate detailed individualised information to reveal specific clinical characteristics and outcome were included. Outcome was dichotomised into either complete recovery (defined as modified Rankin Scale score of zero) or incomplete recovery at final follow-up, assessed in each patient by three independent reviewers (S.B., M.L. and R.C.D.). In the present study we conducted a secondary analysis of this cohort to extract catatonic features using the validated screening instrument of the Bush-Francis Catatonia Rating Scale (BFCRS), comprising a checklist of 14 features in which the presence of ≥2 suggests a diagnosis of catatonia.Reference Bush, Fink, Petrides, Dowling and Francis8 The BFCRS was applied to reports containing adequate detailed descriptions of movement and behaviour by two independent reviewers (S.B. and A.K.). The Mann–Whitney U-test was used to analyse group differences in BFCRS total score according to dichotomised clinical characteristics. Multivariate logistic regression was used to determine the independent association of BFCRS total score with complete recovery.
Results
In total, the cases of 57 patients were analysed (median age 8 years, range 1.3–17; 40 females). A median of three catatonic features were identified per patient (range 0.5–10). Figure 1 details the frequency of each feature within the cohort, and co-occurrences of feature pairs within individual patients (shown as connections between features). Two or more catatonic features were present in 49/57 patients (86%), of whom 34 (69%) had both positive and negative features, 10 (20%) had positive features only, and 5 (10%) had negative features only.
Catatonia was recognised by the reporting physician in only 16/49 patients (33%). Patients with recognised catatonia were older (median 14.5 v. 7 years, P < 0.001) and had a greater number of positive (median 2 v. 1, P = 0.034) and negative (3 v. 1.5, P < 0.001) catatonic features. Five (31%) were treated with lorazepam, without sustained response. Eleven (69%) were treated with antipsychotic medications, with adverse effects reported in five (45%): central nervous system depression and extrapyramidal signs with haloperidol (n = 3), worsening dystonia with olanzapine (n = 1), and orofacial dyskinesia with risperidone (n = 1). In all patients, symptoms of catatonia improved only after initiation of immunotherapy.
Associations of clinical characteristics with catatonia score are detailed in Table 1. Higher catatonia score was associated with a clinical history of prodromal infectious illness (median score 4 v. 3, P = 0.03) and complete recovery from NMDARE (4 v. 3, P = 0.009). Complete recovery occurred in 25/57 patients (44%). There was no significant difference in follow-up duration between those with complete recovery (median 7 months, interquartile range (IQR) = 4.5–17, range 2–54) and those without (median 9 months, IQR = 3–18.75, range 1.3–33) (P = 0.764). To evaluate the independent association of catatonia score with complete recovery (controlling for differences in age and other clinical characteristics) we fitted a multivariate logistic regression model (Supplementary Table 1 available at https://doi.org/10.1192/bjo.2020.55). The presence of each additional catatonic feature (+1 BFCRS score) was associated with 2.08 (CI 1.20–3.60) times increased odds of complete recovery (P = 0.009).
MRI, magnetic resonance imaging.
a. Electroencephalogram was abnormal in all 34 patients with data reported, and therefore not included in the analysis.
b. Delusions, paranoia, hallucinations or thought disorder reported at any time.
c. At presentation to hospital.
d. >5 leucocytes/μL in cerebrospinal fluid (CSF).
Discussion
In total, 86% of children and adolescents with NMDARE had signs and symptoms consistent with catatonia, in keeping with previous reports of catatonia in 19–88% of NMDARE patients.Reference Herken and Pruss4,Reference Espinola-Nadurille, Flores-Rivera, Rivas-Alonso, Vargas-Cañas, Fricchione and Bayliss6,Reference Rogers, Pollak, Blackman and David7 The symptomatology was complex, with 69% of affected patients manifesting both positive (hyperkinetic) and negative (hypokinetic) features. Only 33% were recognised as catatonic by the reporting physician. These were predominantly neurologists, who may tend to interpret movement disorders within a purely neurological paradigm, failing to recognise catatonia as a neuropsychiatric syndrome bridging across traditional symptom domains. Catatonia is not an aetiological diagnosis, but rather a psychomotor dysregulation syndrome with many causes; determination of the cause in the individual patient is of key clinical importance.
Symptomatic treatment with lorazepam was ineffective in this cohort, in keeping with previous reports in adult NMDARE,Reference Espinola-Nadurille, Flores-Rivera, Rivas-Alonso, Vargas-Cañas, Fricchione and Bayliss6 and in contrast to the majority of patients presenting to general psychiatry with catatonia, 88% of whom improve with lorazepam.Reference Walther, Stegmayer, Wilson and Heckers9 Lorazepam acts by potentiating the effect of the inhibitory neurotransmitter γ-amino-butyric acid (GABA) at the GABA-A receptor;Reference Riss, Cloyd, Gates and Collins10 the hypothesised inactivation of GABAergic neurons in NMDAREReference Dalmau, Lancaster, Martinez-Hernandez, Rosenfeld and Balice-Gordon11 may explain the reduced efficacy of the drug in this disease. Failure to respond to lorazepam should therefore prompt careful evaluation for an underlying neurobiological disorder in patients who are catatonic. Adverse effects of antipsychotics occurred in 45% of those treated, in keeping with previous reports in paediatric NMDARE.Reference Mohammad, Jones, Hong, Nosadini, Sharpe and Pillai12 The reasons for this remain unclear, but likely result from complex interactions of cortical and subcortical NMDAR hypofunction with dopaminergic and other neurotransmitter pathways, confounded by a host of other factors experienced by the critically ill patient. The only effective intervention for catatonia in this cohort was early initiation of immunotherapy.
In our exploratory analysis of clinical characteristics associated with catatonia, contrary to previous reports of worse outcome in paediatric NMDARE with catatonia,Reference DeSena, Greenberg and Graves13 we surprisingly found complete recovery was associated with a greater number of catatonic features during the illness course. This is consistent with findings in adults with NMDARE, in which both status epilepticus and death occurred more often in patients without catatonia.Reference Espinola-Nadurille, Flores-Rivera, Rivas-Alonso, Vargas-Cañas, Fricchione and Bayliss6 Recent research implicates dysregulation and hyperactivity of the cortical supplementary and presupplementary motor areas as a pathophysiological mechanism in catatonia;Reference Walther, Stegmayer, Wilson and Heckers9 it may be that patients who are more severely encephalopathic (who tend to have worse outcome) are unable to support any organised output of cortical motor circuits, and so are unable to manifest the behavioural signs of catatonia.
This retrospective study has a number of limitations, including scarcity of detailed information available in case reports for catatonia scoring, bias towards atypical cases in such reports, variable terminology used by authors (typically non-psychiatrists) to describe psychomotor signs and symptoms, and diagnosis that was not always confirmed with cerebrospinal fluid testing. In addition, our analysis of associations with clinical features was exploratory and uncontrolled for multiple comparisons. In summary, we found features consistent with catatonia were highly prevalent in paediatric NMDARE. Catatonia was characterised by mixed or fluctuating symptomatology, resistance to lorazepam and antipsychotic intolerance. Symptoms resolved only with immunotherapy in all cases, highlighting the importance of prompt recognition and treatment of the underlying cause of catatonia.
Supplementary material
Supplementary material is available online at http://doi.org/10.1192/bjo.2020.55
Data availability
The search criteria and papers included in our previously reported systematic literature review are provided in Appendix e-1 of Byrne et al.Reference Byrne, Walsh, Hacohen, Muscal, Jankovic and Stocco5
Acknowledgements
Thanks to Eleni Miltsiou, Victoria Chapman, Helen Barry and Peter Hindley for contributing to ideas highlighted in this study.
Author contributions
M.E. contributed to data analysis and wrote the first draft of the manuscript. A.K. contributed to study formulation/design and data collection. E.B. and M.D.K. contributed to study formulation/design. T.P. contributed to data analysis. R.C.D. contributed to data collection and data analysis. S.B. and M.L. contributed to study formulation/design, data collection and data analysis. All authors contributed to data interpretation and drafting, revising and approving the final manuscript.
Declaration of interest
M.E. reports a travel grant from Terumo BCT, outside the submitted work. R.C.D. reports honoraria from Biogen Idec and Merck Serono as invited speaker, outside the submitted work. M.L. reports personal fees from the Advisory Board Octopharma, and non-financial support from Advisory Board CSL Behring, outside the submitted work. A.K., E.B., M.D.K., T.P. and S.B. report no disclosures.
ICMJE forms are in the supplementary material, available online at https://doi.org/10.1192/bjo.2020.55
eLetters
No eLetters have been published for this article.