Immune Mechanisms in Epileptogenesis: Update on Diagnosis and Treatment of Autoimmune Epilepsy Syndromes

Flammer, Julia; Neziraj, Tradite; Rüegg, Stephan; Pröbstel, Anne‐Katrin

doi:10.1007/s40265-022-01826-9

Cited by 10 publications

(6 citation statements)

References 240 publications

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“…In addition to anti-LGI1 encephalitis, pilomotor seizures have been reported in association with anti-GAD65, anti-NMDAR, anti-Hu, and anti-Ma2 autoimmune and paraneoplastic encephalitides. 1,13 The cellular mechanisms of epileptogenesis in these different immune-mediated encephalitides vary substantially, 14 and it is unlikely that the marked effectiveness of acetazolamide observed in the patients in this series would be expected in patients with pilomotor seizures resulting from other, cellularly unrelated etiologies. Another consideration is whether the functional neuroanatomy of pilomotor seizures, presumed to involve the hypothalamus and central autonomic network, 10,15 might be relevant to pH hypersensitivity and acetazolamide responsiveness.…”

Section: Discussionmentioning

confidence: 89%

“…The LGI1 protein is expressed next to the VGKC Kv1.1, connecting ADAM23 to ADAM22, which are its presynaptic and postsynaptic receptors, respectively. 14 Antibodies against LGI1 have been shown to contribute to temporal lobe epileptogenicity by reducing Kv1 currents and increasing cellular excitability in dentate gyrus granule cells, CA1 and CA3 neurons. 16,17 Although the interaction between acetazolamide and LGI1-related pathology is unclear, it is noteworthy that other channelopathies affecting Kv1.1 have been reported to be acetazolamide responsive, including episodic ataxia type 1.…”

Section: Discussionmentioning

confidence: 99%

“…Most probably there is an unknown interaction between acetazolamide and the underlying pathogenesis of temporal lobe seizures in anti‐LGI1 AE. The LGI1 protein is expressed next to the VGKC Kv1.1, connecting ADAM23 to ADAM22, which are its presynaptic and postsynaptic receptors, respectively 14 . Antibodies against LGI1 have been shown to contribute to temporal lobe epileptogenicity by reducing Kv1 currents and increasing cellular excitability in dentate gyrus granule cells, CA1 and CA3 neurons 16,17 .…”

Section: Discussionmentioning

confidence: 99%

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Acetazolamide as an effective treatment for pilomotor seizures in autoimmune encephalitis

Gilani,

Tarazi,

Wennberg

2024

Epilepsia

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Pilomotor seizures are strongly associated with autoimmune encephalitis (AE), particularly anti‐LGI1 encephalitis. The carbonic anhydrase inhibitor acetazolamide may have special efficacy for treating AE‐associated pilomotor seizures. Six patients with AE (five anti‐LGI1, one seronegative) and temporal lobe pilomotor seizures (five with seizures inducible by hyperventilation) were treated with acetazolamide, administered in a cycling (2‐days‐ON, 4‐days‐OFF) regimen to offset tolerance. Seizures were assessed during epilepsy monitoring unit (EMU) recordings in four inpatients (one of whom also maintained an outpatient seizure diary chronicling 1203 seizures over 1079 days); two outpatients self‐reported seizure frequencies. The extended diary revealed an inverse correlation between acetazolamide and proportion of seizures/day: 6%, 2% (days 1, 2 ON); 3%, 13%, 31%, 45% (days 1, 2, 3, 4 OFF). This patient later developed focal status epilepticus upon wean of antiseizure medications during a seropositive AE relapse that was remarkably aborted with acetazolamide monotherapy. The other three EMU patients averaged .56 seizures/day ON, and 3.81 seizures/day OFF (p = .004). The two outpatients reported seizure reductions from 3–5/day to 2/week, and 15–20/day to none, respectively, after initiation of cycling acetazolamide. Likely related to cerebral CO2/pH sensitivity, acetazolamide can be unusually effective in controlling pilomotor seizures in AE, chronically or in acute settings.

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Section: Discussionmentioning

confidence: 89%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Acetazolamide as an effective treatment for pilomotor seizures in autoimmune encephalitis

Gilani,

Tarazi,

Wennberg

2024

Epilepsia

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“…Both innate and adaptive immunity may be involved in epilepsy [ 53 , 54 ] and a wide range of immune-mediated epilepsies have been identified, although the proportion of individuals with immune-mediated epilepsy is low overall (4‒8%) [ 55 – 57 ]. ASMs are often unsuccessful in controlling seizures in immune-mediated epilepsy [ 58 , 59 ], and PER may therefore be at least as effective as other ASMs in this setting. Treatment should target the underlying cause of immune system dysregulation and early diagnosis of the cause of immune-mediated seizures is required in order to ensure that appropriate treatment is initiated as soon as possible; for example, it is important to identify acute symptomatic seizures secondary to autoimmune encephalitis, since this has well-defined diagnostic criteria and requires early treatment with immunotherapy, including first-line treatment with high-dose intravenous corticosteroids, with or without intravenous immunoglobulins or plasma exchange [ 59 ].…”

Section: Discussionmentioning

confidence: 99%

Perampanel for Treatment of People with a Range of Epilepsy Aetiologies in Clinical Practice: Evidence from the PERMIT Extension Study

Strzelczyk,

Maschio,

Pensel

et al. 2024

Neurol Ther

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Introduction It is important to assess the effectiveness of an antiseizure medication in treating different epilepsy aetiologies to optimise individualised therapeutic approaches. Data from the PERaMpanel pooled analysIs of effecTiveness and tolerability (PERMIT) Extension study were used to assess the effectiveness and safety/tolerability of perampanel (PER) when used to treat individuals with a range of epilepsy aetiologies in clinical practice. Methods A post hoc analysis was conducted of PERMIT Extension data from individuals with a known aetiology. Retention was assessed after 3, 6 and 12 months. Effectiveness was assessed after 3, 6 and 12 months and at the last visit (last observation carried forward). Effectiveness assessments included responder rate (≥ 50% seizure frequency reduction) and seizure freedom rate (no seizures since at least the prior visit). Safety/tolerability was assessed by evaluating adverse events (AEs) and AEs leading to discontinuation. Results PERMIT Extension included 1945 individuals with structural aetiology, 1012 with genetic aetiology, 93 with an infectious aetiology, and 26 with an immune aetiology. Retention rates at 12 months were 61.1% (structural), 65.9% (genetic), 56.8% (infectious) and 56.5% (immune). At the last visit, responder rates (total seizures) were 43.3% (structural), 68.3% (genetic), 37.0% (infectious) and 20.0% (immune), and corresponding seizure freedom rates were 15.8%, 46.5%, 11.1% and 5.0%, respectively. AE incidence rates were 58.0% (structural), 46.5% (genetic), 51.1% (infectious) and 65.0% (immune), and corresponding rates of discontinuation due to AEs over 12 months were 18.9%, 16.4%, 18.5% and 21.7%, respectively. The types of AEs reported were generally consistent across aetiology subgroups, with no idiosyncratic AEs emerging. Conclusion Although PER was effective and generally well tolerated when used to treat individuals with a range of epilepsy aetiologies in clinical practice, variability in its effectiveness and tolerability across the subgroups indicates that PER may be particularly useful for individuals with specific epilepsy aetiologies. Supplementary Information The online version contains supplementary material available at 10.1007/s40120-024-00618-5.

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“… 12 , 13 As a result, there would be less GABA available in the synaptic cleft and more presynaptic glutamate. 14 …”

Section: Introductionmentioning

confidence: 99%

Cenobamate and Clobazam Combination as Personalized Medicine in Autoimmune-Associated Epilepsy With Anti-Gad65 Antibodies

Serrano-Castro,

Rodríguez-Uranga,

Cabezudo-García

et al. 2023

Neurol Neuroimmunol Neuroinflamm

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Background and ObjectivesAutoimmune-associated epilepsy (AAE) with antiglutamic acid decarboxylase 65 (GAD65) antibodies is considered a T-cell–mediated encephalitis that evolves to drug-resistant epilepsy. We do not have an effective therapeutic strategy for these patients. Because the GAD enzyme is primarily responsible for the conversion of glutamate to GABA, the mechanism of epileptogenesis in this condition predicts decreased levels of GABA content in synaptic vesicles. Cenobamate (CNB) acts as a positive allosteric modulator at synaptic and extra synaptic GABAA receptors, producing increased inhibitory neurotransmission in the brain. This mechanism could be especially beneficial in AAE with anti-GAD65 antibodies because it would be able to correct the imbalance due to the GABAergic stimulation deficit in postsynaptic neurons.MethodsWe recruit a retrospective multicentric consecutive case series of AAE with anti-GAD65 antibodies from 5 epilepsy units in Spain who have received treatment with CNB.ResultsA total of 8 patients were recruited. This cohort of highly refractory patients have failed a mean of 9.50 (SD = 3.20) ASM without control of seizures for sustained periods of time. The average number of seizures per month during the previous 3 months before CNB treatment was 19.63 (SD = 17.03). After the introduction of CNB improvement was achieved in all our patients, with a median reduction in the number of seizures of 92.22% (interquartile range [IQR]: 57.25–98.75). The mean follow-up was 156.75 days (SD = 68.23). In patients with concomitant treatment with clobazam (CLB), the median percentage of seizure reduction was higher than those not taking CLB: 94.72% (IQR: 87.25–100) vs 41.50% (p= 0.044) and also higher than the control group of patients with refractory epilepsy not related to anti-GAD65 treated with the same combination: 94.72% (IQR: 87.25–100) vs 45.00% (IQR: 25.00–87.00) (p= 0.019).DiscussionTreatment with the combination CNB + CLB could be a type of personalized medicine in patients with AAE with anti-GAD65. Our preliminary data will need to be endorsed with new prospective and controlled studies.

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Immune Mechanisms in Epileptogenesis: Update on Diagnosis and Treatment of Autoimmune Epilepsy Syndromes

Cited by 10 publications

References 240 publications

Acetazolamide as an effective treatment for pilomotor seizures in autoimmune encephalitis

Acetazolamide as an effective treatment for pilomotor seizures in autoimmune encephalitis

Perampanel for Treatment of People with a Range of Epilepsy Aetiologies in Clinical Practice: Evidence from the PERMIT Extension Study

Cenobamate and Clobazam Combination as Personalized Medicine in Autoimmune-Associated Epilepsy With Anti-Gad65 Antibodies

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