In their Praxis article, Beattie and colleagues present a case of anti-N-methyl-d-aspartate receptor (anti-NMDAR) encephalitis and make suggestions for psychiatrists on how to approach such difficult clinical situations.Reference Beattie, Goodfellow, Oto and Krishnadas1 The importance of this topic to psychiatrists lies in the fact that although anti-NMDAR encephalitis is primarily a neurological disorder, nearly 80% of these patients first present with psychiatric symptoms and more than 60% are first admitted to psychiatric units.Reference Bost, Pascual and Honnorat2 It is estimated that nearly 75% of these individuals recover or have minimal deficits, although up to 25% endure severe functional deficits or even die, mostly owing to delays in diagnosis.Reference Dalmau, Gleichman, Hughes, Rossi, Peng and Lai3 Hence, early recognition and treatment are key to a successful outcome.
The clinical case described by Beattie and colleagues is of a woman in her mid-20s treated initially for a psychiatric disorder who later developed neurological deficits raising suspicion of anti-NMDAR encephalitis. The authors demonstrate the challenges likely to occur in clinical situations when there is the potential for being misled by the initial emergence of psychiatric symptoms as early manifestation of this disease. Following a systematic approach to clinical reasoning might help to consider the possibility of anti-NMDAR encephalitis as early as possible.Reference Abdel Aziz, AlSuwaidi, Al-Ammari, Al Khoori, AlBloushi and Al-Nuaimi4 Early cues are an important element in increasing the chance of early diagnosis of anti-NMDAR encephalitis, essential to improve outcome. Beattie and colleagues highlight the importance of ‘red flags’ to aid the diagnosis of autoimmune encephalitis. These red flags include a host of associated manifestations that could aid early diagnosis, especially when detecting for the presence of autoantibodies, central to diagnosis and treatment of anti-NMDAR encephalitis, is not feasible. This editorial provides a succinct description of the several types of autoantibodies associated with autoimmune encephalitis and highlights the difficulties in reaching the diagnosis and providing treatment.
Autoimmune encephalitis and autoantibody subtypes
Anti-NMDAR encephalitis is the most frequently occurring of several types of autoimmune encephalitis.Reference Huang and Xiong5 It affects around 1.5 per million people/year.Reference Dalmau, Armangué, Planagumà, Radosevic, Mannara and Leypoldt6 Autoimmune encephalitides are broadly divided into two categories according to whether the immunological mechanism involves autoantibodies targeting ‘extracellular’ or ‘intracellular’ neuronal antigens. The overall incidence has increased from 0.4/100 000 in 1995–2005 to 1.2/100 000 in 2006–2015.Reference Dubey, Pittock, Kelly, McKeon, Lopez-Chiriboga and Lennon7 This could be explained by changes in consensus definitions, which initially focused on neuronal surface autoantibody-mediated encephalopathies and only subsequently included paraneoplastic limbic and anti-voltage-gated potassium channel antibodies.
There is a crucial distinction between paraneoplastic syndromes associated with onconeural antibodies and other autoimmune encephalopathies. Onconeural antibodies against surface antigenic targets are in fact biomarkers with no bearing on the disease process, unlike the more common autoimmune encephalitides. Onconeural antibodies against intracellular targets represent malignancy.
Autoantibodies that often target extracellular receptors and ion channels include those for NMDA (N-methyl-d-aspartate), AMPA (α-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid), GABA (gamma-aminobutyric acid), glycine receptors, and voltage-gated potassium channels (VGKC) including LGI1 (leucine-rich glioma inactivated 1) and CASPR2 (contactin-associated protein-like 2) proteins.Reference Dalmau and Graus8 Autoantibodies that target either intracellular antigens or synaptic proteins include anti-Hu, anti-Ri, anti-Yo, anti-Ma, anti-amphiphysin and anti-GAD (glutamic acid decarboxylase). The immune response that targets intracellular antigens is thought to involve CD8+ cytotoxic T-cell-mediated cell injury after binding of autoantibodies to the target intracellular antigen. These autoimmune encephalitides are often paraneoplastic manifestations of various types of cancer.Reference Deng and Yeshokumar9,Reference Lancaster10
Although psychiatric symptomatology can occur with any antibody-positive encephalitis, it is more frequent in presentations associated with autoantibodies targeting extracellular antigens.Reference Hansen and Timäus11
Autoantibodies targeting extracellular antigens
Anti-NMDAR encephalitis
NMDA receptors are glutamatergic ionotropic receptors often found in the presynaptic GABA neurons of the thalamus and frontal lobes. Impairment of these receptors leads to dysfunction of glutamatergic and dopaminergic networks throughout the brain.Reference Dalmau and Graus8
Animal studies suggest that anti-NMDA receptors passively transferred into the brains of rodents produce neurological symptoms proportionate to the surface reduction of NMDA receptors on the neurons,Reference Planagumà, Leypoldt, Mannara, Gutiérrez-Cuesta, MartínGarcía and Aguilar12 causing depletion of NMDA receptors from the synapse.Reference Moscato, Jain, Peng, Hughes, Dalmau and Balice-Gordon13 This depletion can explain the insurgence of psychotic symptoms experienced by patients (early confusion, psychosis, visual hallucinations and personality change, followed by neurological deficits),Reference Deng and Yeshokumar9 which is analogous to psychotic manifestations observed with phencyclidine ingestion, which also acts through NMDA receptor hypofunction.Reference Lancaster10
Anti-AMPAR encephalitis
AMPA receptors are also glutamatergic ionotropic receptors that are widely expressed in the brain mediating rapid excitatory transmission.Reference Lancaster10 Anti-AMPAR encephalitis tends to present with psychiatric symptoms similar to anti-NMDAR encephalitis. The median age at onset of this type of encephalitis tends to be in the 40s and 50s,Reference Dalmau and Graus8,Reference Lai, Hughes, Peng, Zhou, Gleichman and Shu14 which differs from anti-NMDAR encephalitis, which mostly affects females in their 20s.Reference Dalmau and Graus8
Anti-LG1 antibody encephalitis
LGI1 is a presynaptic glycoprotein involved in the regulation of AMPA and VGKC receptors. On cultured neurons, LGI1 antibodies have been shown to affect AMPA receptor localisation across the whole brain. Classic symptoms of anti-LGI1 antibody encephalitis include hyponatraemia and faciobrachial dystonic seizures with initial subtle memory loss and sleep disorders (hypersomnia, insomnia, rapid-eye movement (REM) sleep behaviour disorder, sleep reversal). This condition tends to occur at a median age of 60 years.Reference Deng and Yeshokumar9,Reference Ohkawa, Fukata, Yamasaki, Miyazaki, Yokoi and Takashima15
CASPR2 antibody encephalitis
CASPR2 is a cell adhesion molecule that organises VGKCs in the central and peripheral nervous system. People with anti-CASPR2 antibodies develop symptoms originating in the central nervous system (limbic encephalitis) and/or the peripheral nervous system (e.g. Morvan syndrome), with encephalitis characterised by confusion, amnesia and hallucinations. Onset is usually slower than for anti-NMDAR encephalitis and the median age at onset is 60 years.Reference Lancaster10,Reference Dalmau and Rosenfeld16
Anti-GABA receptor encephalitis
GABA is the primary inhibitory ionotropic receptor in the brain. Antibodies targeting GABAA and GABAB receptors result in a type of limbic encephalitis associated with severe seizures that can lead to status epilepticus, together with psychiatric manifestations such as memory loss, confusion, hallucinations and personality change.Reference Lancaster, Lai, Peng, Hughes, Constantinescu and Raizer17–Reference Höftberger, Titulaer, Sabater, Dome, Rózsás and Hegedus19
Glycine-receptor autoantibody-associated disease
The glycine receptor is an inhibitory receptor. The α1 subunit is the predominant antigenic target.Reference Martinez-Hernandez, Arino, McKeon, Iizuka, Titulaer and Simabukuro20 Studies involving the transfer of human glycine autoantibodies to rodents have demonstrated that neural transmission at the cellular level with consecutive, altered signal cascades induces psychiatric and cognitive symptoms. Glycine-receptor antibodies have been found in ‘stiff person spectrum’ disorders such as progressive encephalomyelitis with rigidity and myoclonus and have been associated with cognitive/memory dysfunction and psychosis.Reference Hansen and Timäus11
Autoantibodies targeting intracellular antigens and proteins
Autoantibodies that target intracellular antigens (anti-Hu, anti-Ri, anti-Ma, anti-Yo) and proteins (anti-amphiphysin, anti-GAD) typically present as paraneoplastic manifestations. Neuropsychiatric symptoms often precede the diagnosis of the primary neoplasia by several months. Common symptoms include depression, irritability, hallucinations, sleep disturbance and seizures. Memory loss can occur over weeks to months, in some cases progressing to severe cognitive decline resembling a dementing illness.Reference Deng and Yeshokumar9 The latter has been associated with anti-Hu antibodies, which target an intracellular RNA-packed protein, important in memory-related synaptic plasticity.Reference Hansen and Timäus11 Anti-Ri antibodies have been linked with lung carcinoma. Typical manifestations include personality changes and neuropsychological deficits.Reference Hansen and Timäus11 Anti-Ma antibodies are often found in young males with germ cell tumours and are associated with a range of psychiatric manifestations, including obsessive–compulsive disorder, delirium, major depression, personality changes and amnesia.Reference Hansen and Timäus11 Anti-Yo antibodies are mostly found in females with breast or ovarian cancers. These antibodies most likely act through T-cell mechanisms and are associated with psychosis.Reference Hansen and Timäus11,Reference Tanaka, Kawamura, Sakimura and Kato21,Reference Greenlee, Clawson, Hill, Wood, Tsunoda and Carlson22
Anti-amphiphysin antibodies are very strongly associated with breast cancer in women. These antibodies target intracellular proteins important for recycling synaptic vesicles. Animal models suggest that in rats, when anti-amphiphysin antibodies are passively transferred intrathecally they can induce anxiety behaviours.Reference Lancaster10,Reference Geis, Grünewald, Weishaupt, Wultsch, Toyka and Reif23 Anti-GAD antibodies target the synaptic isoform of the enzyme necessary to synthesise GABA.Reference Lancaster10 Mood changes and cognitive impairment are the most frequent symptoms.Reference Hansen and Timäus11
Summary
Although anti-NMDAR encephalitis is the most common of the autoimmune encephalitides, there are several other types of autoantibody targeting extracellular and intracellular antigens that can present with similar clinical characteristics. In the presence of atypical, often rapidly evolving psychiatric manifestations, especially when coexisting with neurological symptoms, an early age at onset in a female patient or a mid to late onset in both genders might raise the suspicion of encephalitis. It is important to consider the possibility of a primary neoplasia and a relatively recent diagnosis of cancer, especially if originating in the ovaries, breast, lung and germ cells.
Autoantibody screening
Beattie and colleagues highlight the complexities of screening and interpreting serum/cerebrospinal fluid (CSF) anti-NMDAR autoantibody levels in patients presenting with psychiatric symptoms. Rates of false positives and false negatives in affected individuals are high, in the range of 10%.Reference Hammer, Stepniak, Schneider, Papiol, Tantra and Begemann24,Reference Gresa-Arribas, Titulaer, Torrents, Aguilar, McCracken and Leypoldt25
Commercial kits are now available for different types of autoantibody other than anti-NMDAR (e.g. LGI1, Caspr2, AMPAR and GABA),Reference Lancaster10 although results may require several weeks of processing. For extracellular antibody tests other than anti-NMDAR encephalitis, CSF is still the most sensitive and specific test, with serum offering a high rate of false-negative results.Reference Lancaster10 In the case of intracellular antibody tests, positive test results on their own might not be sufficient as definitive confirmation of a particular autoimmune aetiology. Some of these autoantibodies, for example anti-GAD65, may be associated with other disorders (e.g. type 1 diabetes) and may coexist with other autoantibodies, for example anti-GABAB.
A recent meta-analysis suggests that in cross-sectional studies NMDAR IgG antibodies are more common in people with psychosis than in controlsReference Cullen, Palmer-Cooper, Hardwick, Vaggers, Crowley and Pollak26 and a further recent study showed the limitations of commercial assays as diagnostic tests for autoimmune encephalitis.Reference Ruiz-García, Muñoz-Sánchez, Naranjo, Guasp, Sabater and Saiz27 Excessive screening based on recognition of the stereotyped clinical syndromes but without sufficient prior probability is controversial. Moreover, although pairing serum with CSF testing can be helpful in correlation with clinical symptoms, it is important to recognise that in some autoimmune encephalitides (e.g. LGI1), autoantibodies are often undetectable in CSF. Furthermore, as these conditions differ epidemiologically (e.g. LGI1 and CASPR2 are exceedingly rare in young people, and NMDAR is rare in older adults) a targeted approach to testing is greatly advisable.
In summary, depending on the laboratory and assay used, autoantibodies can be detected outside of the canonical clinical syndromes and overinterpreting these results can cause harm. In view of this uncertainty and the possibility that immunotherapy might be effective, the recent consensus is to consider a diagnosis of ‘seronegative autoimmune encephalitis’ in the presence of clinical symptoms and absence of autoantibodies.Reference Ellul, Wood, Tooren, Easton, Babu and Michael28
Implications for diagnosis and treatment
Diagnostic uncertainty, highly disturbed mental states, logistic difficulties in carrying out a range of essential investigations (lumbar puncture, electroencephalogram and magnetic resonance imaging) can delay the prospective identification of these conditions, particularly in undifferentiated psychiatric services. The use of screening criteria for anti-NMDAR encephalitis can help improve the detection of autonomic dysfunction, cognitive impairment and movement disorders, but ‘red flag’ symptoms tend to overlap with those seen in functional psychiatric illness.Reference Warren, Flavell, O'Gorman, Swayne, Blum and Kisely29
Currently there is no definitive treatment algorithm for anti-NMDAR encephalitis. Recommended initial therapy includes intravenous immunoglobulins and methylprednisolone or daily plasma exchange. For refractory illness, second-line treatments include rituximab and cyclophosphamide. The proteasome inhibitor bortezomib has shown some efficacy in highly refractory disease.Reference Titulaer, McCracken, Gabilondo, Armangué, Glaser and Iizuka30,Reference Simmons and Perez31 Similar immunosuppressant strategies can be used for the other types of extracellular autoimmune encephalitis. Anti-LGI1 encephalitis generally responds well to first-line treatment,Reference Ellul, Wood, Tooren, Easton, Babu and Michael28 and rituximab is thought to be generally effective where the autoantibodies are of the IgG4 subtype, which predominate in anti-LGI1 and anti-CASPR2 encephalitides.Reference Lancaster10
Patients with clinical symptoms due to autoantibodies targeting intracellular antigens are believed to respond poorly to immunotherapy. This is possibly related to CD8+ mediated cytotoxicity, which may cause irreversible neuronal cell injury. For these patients prompt detection and treatment of the underlying neoplasm is the best approach for symptom resolution.Reference Ellul, Wood, Tooren, Easton, Babu and Michael28
In summary, there is variability in the approach to diagnosis and treatment of autoimmune encephalitis often driven by the specialty of the assessing clinician rather than the clinical presentation. Hence, for suspected cases there is great need to collaborate with local neurologists to establish preferential diagnostic pathways involving regional neuroscience centres where systematic diagnostic assessment and investigations can be facilitated. Immunosuppressant strategies are considered the most effective treatment of extracellular types of autoimmune encephalitis, whereas identifying and treating the cancerous source of paraneoplastic symptoms is the most effective approach for the type of autoimmune encephalitis targetting intracellular antigens.
Conclusions
The presence of autoantibodies against brain receptors or proteins can result in severe yet potentially treatable autoimmune encephalitis. Detecting autoantibodies is a necessary but not always informative diagnostic step. History or suspicion of cancer should alert clinicians. Atypical psychiatric manifestations, commonly associated with neurological symptoms, raise concerns about the origin of these disorders. The clinical distinction between autoimmune encephalitis and psychiatric presentations is very challenging. The use of screening tools and preferential diagnostic pathways in collaboration with local neurologists with access to regional neuroscience centres could facilitate reaching a timely diagnosis.
About the authors
Karim Abdel Aziz is an Associate Professor in the Department of Psychiatry, College of Medicine and Health Sciences, United Arab Emirates University (UAEU), Al-Ain, UAE. Emmanuel Stip is a Professor and Chair of the Department of Psychiatry, College of Medicine and Health Sciences, UAEU, Al-Ain, UAE; he is also Professor Emeritus of Psychiatry in the Department of Psychiatry, Institute Universitaire en Santé Mentale de Montréal, Université de Montréal, Canada. Danilo Arnone is an Associate Professor in the Department of Psychiatry, College of Medicine and Health Sciences, UAEU, Al-Ain, UAE; he is also affiliated with the Centre for Affective Disorders, Institute of Psychiatry, Psychology and Neuroscience, King's College London, UK.
Data availability
Data availability is not applicable to this article as no new data were created or analysed in this study.
Author contributions
K.A.A. wrote the first draft and contributed to subsequent versions of the manuscript. E.S. contributed to writing the manuscript and subsequent revisions. D.A. conceived the idea and contributed to the writing leading to final acceptance.
Funding
This research received no specific grant from any funding agency, commercial or not-for-profit sectors.
Declaration of interest
D.A. has received travel grants from Janssen-Cilag and Servier and sponsorship from Lundbeck.
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