Clinical features which predict neuronal surface autoantibodies in new-onset focal epilepsy: implications for immunotherapies

McGinty, Ronan N.; Handel, Adam E.; Moloney, Teresa C.; Ramesh, Archana; Fower, Andrew; Torzillo, Emma; Kramer, Holger; Howell, Stephen; Waters, Patrick; Adcock, Jane; Sen, Arjune; Lang, Bethan; Irani, Sarosh R.

doi:10.1136/jnnp-2020-325011

Cited by 36 publications

(44 citation statements)

References 15 publications

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“…However, only recently have studies combined accurate clinical phenotyping with the autoantibody results in unselected populations. 23 24 These largely concur with our routine clinical experience: patients who have unselected new-onset seizures, neuronal surface autoantibodies and an immunotherapy-responsive syndrome typically have mild features of autoimmune encephalitis, such as cognitive and mood features, specific seizure semiologies, dysautonomia and limbic MRI changes. This clinically-driven assessment approach aims to limit unfruitful or equivocal immunotherapy trials in patients attending epilepsy clinics.…”

Section: Seizuressupporting

confidence: 78%

Autoimmune encephalitis: clinical spectrum and management

2021

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Autoimmune encephalitis defines brain inflammation caused by a misdirected immune response against self-antigens expressed in the central nervous system. It comprises a heterogeneous group of disorders that are at least as common as infectious causes of encephalitis. The rapid and ongoing expansion of this field has been driven by the identification of several pathogenic autoantibodies that cause polysymptomatic neurological and neuropsychiatric diseases. These conditions often show highly distinctive cognitive, seizure and movement disorder phenotypes, making them clinically recognisable. Their early identification and treatment improve patient outcomes, and may aid rapid diagnosis of an underlying associated tumour. Here we summarise the well-known autoantibody-mediated encephalitis syndromes with neuronal cell-surface antigens. We focus on practical aspects of their diagnosis and treatment, offer our clinical experiences of managing such cases and highlight more basic neuroimmunological advances that will inform their future diagnosis and treatments.

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Section: Seizuressupporting

confidence: 78%

Autoimmune encephalitis: clinical spectrum and management

2021

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“…For instance, focal epileptic seizures or behavioral changes may occur in isolation at onset but often evolve rapidly to status epilepticus and/or encephalopathy, which can help diagnostically to distinguish from isolated epilepsy, psychiatric disorders, or typical neurodegenerative dementia (30)(31)(32). Different scoring systems have been designated to help clinicians determine the likelihood of autoantibody detection in patients with different neurological manifestations (33)(34)(35). Viral-like prodromes or vaccinations are not uncommon at or before symptom onset (26)(27)(28)36).…”

Section: Identification Of Compatible Clinical-mri Phenotypesmentioning

confidence: 99%

Antibody-Mediated Autoimmune Diseases of the CNS: Challenges and Approaches to Diagnosis and Management

Sechi

Flanagan

2021

Front. Neurol.

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Antibody-mediated disorders of the central nervous system (CNS) are increasingly recognized as neurologic disorders that can be severe and even life-threatening but with the potential for reversibility with appropriate treatment. The expanding spectrum of newly identified autoantibodies targeting glial or neuronal (neural) antigens and associated clinical syndromes (ranging from autoimmune encephalitis to CNS demyelination) has increased diagnostic precision, and allowed critical reinterpretation of non-specific neurological syndromes historically associated with systemic disorders (e.g., Hashimoto encephalopathy). The intracellular vs. cell-surface or synaptic location of the different neural autoantibody targets often helps to predict the clinical characteristics, potential cancer association, and treatment response of the associated syndromes. In particular, autoantibodies targeting intracellular antigens (traditionally termed onconeural autoantibodies) are often associated with cancers, rarely respond well to immunosuppression and have a poor outcome, although exceptions exist. Detection of neural autoantibodies with accurate laboratory assays in patients with compatible clinical-MRI phenotypes allows a definite diagnosis of antibody-mediated CNS disorders, with important therapeutic and prognostic implications. Antibody-mediated CNS disorders are rare, and reliable autoantibody identification is highly dependent on the technique used for detection and pre-test probability. As a consequence, indiscriminate neural autoantibody testing among patients with more common neurologic disorders (e.g., epilepsy, dementia) will necessarily increase the risk of false positivity, so that recognition of high-risk clinical-MRI phenotypes is crucial. A number of emerging clinical settings have recently been recognized to favor development of CNS autoimmunity. These include antibody-mediated CNS disorders following herpes simplex virus encephalitis or occurring in a post-transplant setting, and neurological autoimmunity triggered by TNFα inhibitors or immune checkpoint inhibitors for cancer treatment. Awareness of the range of clinical and radiological manifestations associated with different neural autoantibodies, and the specific settings where autoimmune CNS disorders may occur is crucial to allow rapid diagnosis and early initiation of treatment.

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“…Some of them are: adult onset of seizures above 30 years old, antiepileptic drug‐resistance, new‐onset refractory status epilepticus, no risk factors for seizures, personal or familiar history of autoimmune diseases, neuropsychiatric changes, autonomic dysfunction, viral prodrome, recent or past neoplasia, or evidence of central nervous system (CNS) inflammation by lumbar puncture or MRI. It is important to highlight that there are no strict criteria to diagnose autoimmune‐associated epilepsy 5,6 …”

Section: Methodsmentioning

confidence: 99%

Brain FDG‐PET findings in glutamic acid decarboxylase antibody‐associated epilepsy

Mongay-Ochoa

Sala-Padró

Reynés-Llompart

et al. 2021

Journal of Neuroimaging

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Background and Purpose Glutamic acid decarboxylase antibodies (GAD‐Ab) are sometimes associated with chronic drug‐resistant focal epilepsy. Clinically, it may manifest as mesial temporal lobe epilepsy (mTLE), with GAD‐Ab patients difficult to distinguish. Therefore, the aim of this study is to compare brain metabolism of patients with mTLE and high serum titers of GAD‐Ab (>2000 UI/ml) to those with mTLE and hippocampal sclerosis (HS) and confirmed GAD‐ab negativity. Methods Images from PET studies were normalized to an SPM 12 template. Voxel to voxel comparisons were made using a two‐sample one‐tailed t‐test. Results In both patients with GAD‐Ab and controls (mTLE‐HS), hypometabolism in mesial temporal lobe areas was observed. When comparing the two groups, GAD‐Ab patients had statistically significant reduced metabolism in both insulae and medial inferior frontal‐hypothalamus area (p < 0.001). Conclusions Hypometabolism in mesial temporal lobe areas together with hypometabolism in insulae and medial inferior frontal‐hypothalamus may be characteristic of patients with epilepsy and GAD‐ab. This PET pattern could be a useful diagnostic tool to identify GAD‐Ab patients.

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Clinical features which predict neuronal surface autoantibodies in new-onset focal epilepsy: implications for immunotherapies

Cited by 36 publications

References 15 publications

Autoimmune encephalitis: clinical spectrum and management

Autoimmune encephalitis: clinical spectrum and management

Antibody-Mediated Autoimmune Diseases of the CNS: Challenges and Approaches to Diagnosis and Management

Brain FDG‐PET findings in glutamic acid decarboxylase antibody‐associated epilepsy

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