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Last updated: 20 June 2024

Familial (Autosomal Dominant) Focal Epilepsies

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Autosomal Dominant Familial Focal EpilepsyAutosomal Dominant Familial Temporal Lobe EpilepsyAutosomal Dominant Rolandic Epilepsy and Speech DyspraxiaFamilial Focal Epilepsy with Variable FociFocal Epilepsy with Pericentral SpikesLateral familial temporal lobe epilepsyMesial familial temporal lobe epilepsy

  • Overview:

    • Temporal lobe epilepsy was traditionally considered an acquired condition.
    • Causes include lesions such as:
      • Hippocampal sclerosis
      • Tumours
      • Trauma
      • Vascular malformations
      • Malformations of cortical development
    • Recent research has highlighted the genetic involvement in some forms of temporal lobe epilepsy.

  • Inheritance:

    • Familial temporal lobe epilepsy is inherited in an autosomal dominant manner.

  • Types:

    • Mesial Familial Temporal Lobe Epilepsy (MFTLE):
      • Characterised by seizure symptomatology typical of mesial temporal lobe epilepsy.
      • Symptoms include:
        • Déjà vu
        • Autonomic phenomena
    • Lateral Familial Temporal Lobe Epilepsy (LFTLE):
      • Also known as partial epilepsy with auditory symptoms.
      • Characterised by subjective ictal symptoms.
      • Symptoms include:
        • Auditory hallucinations originating from the lateral temporal lobe.

  • Onset and Nature:

    • Both MFTLE and LFTLE typically begin in adolescence or adult life.
    • These forms of epilepsy are usually considered benign epilepsy syndromes.

Mesial Familial Temporal Lobe Epilepsy (MFTLE)

  • Overview:

    • MFTLE is an autosomal dominant epileptic disease.
    • Onset typically occurs in teenage or early adult life.
    • Median onset is in the middle of the third decade of life.
    • No cases have been identified in children under 10 years.
    • Women may be affected more than men (58%).
    • Epidemiology is unknown, but it may be a common condition.

  • Clinical Manifestations:

    • Seizures are generally mild, infrequent, and well controlled with antiepileptic drugs (AEDs).
    • Seizure Types:
      • Simple focal seizures (90%) are more common than complex focal seizures (66%).
      • Simple focal seizures may be the only seizure type (18%).
    • Ictal Symptoms:
      • Déjà vu
      • Experiential phenomena and hallucinations
      • Autonomic disturbances
      • Emotional symptoms (fear and panic)
      • Visual and auditory illusions
      • Somatosensory sensations (diffuse numbness and tingling)
    • Generalized Tonic-Clonic Seizures (GTCS):
      • Occur in only two-thirds of patients.
      • In 50% of cases, GTCS occur before appropriate treatment is initiated.
      • Infrequent, with a worst-case scenario of one GTCS per year.

  • Aetiology:

    • Autosomal dominant inheritance with reduced penetrance (60%).
    • The responsible gene has not yet been identified.

  • Diagnostic Procedures:

    • MRI:
      • Often normal but may show hippocampal atrophy in severe cases.
      • Minor, non-specific abnormalities (diffuse, small, high signal areas on T2-weighted images).
    • Interictal FDG-PET:
      • May show ipsilateral temporal hypometabolism in patients with active seizures.
    • EEG:
      • Interictal EEG is usually normal (50% of cases).
      • May show mild, focal, slow waves (28%) or sparse, unilateral sharp and slow wave complexes (22%).
      • Sleep may occasionally activate epileptiform abnormalities.

  • Differential Diagnosis:

    • Differentiating from normal phenomena in cases with mild and infrequent seizures of predominantly déjà vu can be challenging.
    • Main differentiating features from hippocampal epilepsy:
      • Onset in teens or early adult life
      • No febrile convulsions or other antecedent factors
      • No ictal symptoms of rising epigastric aura
      • Mild and infrequent seizures that may remit
      • Usually normal MRI

  • Prognosis:

    • Generally good prognosis.
    • One-sixth of cases with mild simple partial seizures alone might be unaware of their condition if not for affected family members.
    • Complex focal seizures and GTCS are infrequent and respond well to AEDs.
    • Rare for seizures to persist after drug treatment (10-20% of cases).
    • Long remissions, with or without therapy, are common.
    • More severe clinical spectrum observed in patients considering surgical treatment.

  • Management:

    • Seizures are usually easily controlled with carbamazepine or phenytoin.
    • Patients with refractory MFTLE have a good surgical outcome when unilateral or clearly asymmetric hippocampal atrophy is identified.
    • Preoperative investigation should be the same as for patients with sporadic refractory MFTLE.

Lateral Familial (Autosomal Dominant) Temporal Lobe Epilepsy (LFTLE)

  • Overview:

    • Also known as "autosomal dominant focal epilepsy with auditory features."
    • Caused by defects in the same gene.
    • First non-ion channel familial epilepsy discovered.
    • Previously discovered genes for idiopathic epilepsies were associated with ion channels.

  • Demographic Data:

    • Onset typically in teenage or early adult life.
    • Can occur as early as 5-10 years of age or later.

  • Clinical Manifestations:

    • Seizure Characteristics:
      • Mild seizures with mainly auditory hallucinations.
      • Mainly nocturnal and infrequent generalized tonic-clonic seizures (GTCS).
      • Excellent response to treatment with antiepileptic drugs (AEDs).
    • Seizure Types:
      • Simple focal seizures are most common.
        • Auditory hallucinations (ringing, humming, clicking, unspecified noises).
        • Other sensory symptoms (visual, olfactory, vertiginous, cephalic).
      • Autonomic, experiential, and motor symptoms are less common.
      • Simple focal seizures may progress to complex focal seizures.
      • Brief aphasic seizures have been described.
    • GTCS:
      • Rare and predominantly nocturnal.

  • Aetiology:

    • Autosomal dominant inheritance with high penetrance (~80%).
    • Linked to chromosome 10q, localizing a gene in a common overlapping region of 3-cM at 10q24 (LGI1/Epitempin gene).
    • LGI1 mutations cause protein truncation, leading to loss of function.
    • LFTLE is genetically heterogeneous; LGI2, LGI3, or LGI4 mutations do not account for all cases.

  • Diagnostic Procedures:

    • EEG and MRI are often normal or show mild, non-specific abnormalities.
    • Interictal EEG epileptiform abnormalities are rare.

  • Prognosis:

    • Excellent prognosis.
    • Patients are neurologically and mentally normal.
    • The condition does not significantly affect normal life, especially with medication.

  • Differential Diagnosis:

    • Differentiated from other structural causes of lateral temporal lobe epilepsy.
    • Different from hippocampal and other types of mesial familial temporal lobe epilepsy (MFTLE).
      • Main ictal symptom of LFTLE: auditory hallucinations.
      • Main ictal symptoms of MFTLE: déjà vu and other experiential phenomena.

  • Management:

    • Excellent response to carbamazepine.

Familial Focal Epilepsy with Variable Foci

  • Overview:

    • Familial partial epilepsy with variable foci is an autosomal dominant syndrome.
    • Characterized by focal seizures originating from different brain regions in different family members.
    • Occurs in the absence of detectable structural abnormalities.

  • Demographic Data:

    • Age at onset varies widely (from months to 43 years).
    • Mean age at onset of seizures is 13 years.
    • Reported in eight unrelated families to date.

  • Clinical Manifestations:

    • Different family members have focal seizures from different cortical locations:
      • Temporal
      • Frontal
      • Centroparietal
      • Occipital
    • Each patient has a consistent electroclinical pattern of single-location focal epilepsy.
    • Seizures are often nocturnal.
    • Great intrafamilial variability in severity:
      • Some are asymptomatic with only an EEG spike-focus.
      • Most are easily controlled with AEDs.
      • A few may be intractable to medication.
    • Identification is challenging in small families due to insufficient individuals to establish a specific pattern.

  • Aetiology:

    • Rare inherited syndrome with autosomal dominant inheritance.
    • Penetrance of about 60%.
    • In two families, mapped to a locus on chromosome 22q11-q12.
    • Genetic heterogeneity indicated by non-linkage to chromosome 22 in the original Australian family and a suggestion of linkage on chromosome 2q.

  • Diagnostic Procedures:

    • Neuroimaging:
      • Usually normal.
    • Electroencephalography (EEG):
      • Interictal focal epileptiform abnormalities occur in most patients.
      • Locations vary between family members but remain constant for each individual over time.
      • Abnormalities often facilitated or brought on by sleep.
      • Clinical seizures align with EEG localization.
      • EEG severity varies among individuals and does not correlate with seizure frequency.
      • Normal family members may also exhibit an EEG spike focus, indicating it as a marker for the syndrome.

  • Prognosis:

    • Development is usually normal.

  • Management:

    • Effects of new AEDs not directly evaluated.
    • Carbamazepine and phenytoin appear to be effective.

Autosomal Dominant Rolandic Epilepsy and Speech Dyspraxia

  • Overview:

    • Described as a rare hereditary condition by the Australian team of Berkovic, Scheffer, and associates.
    • Characterized by nocturnal oro-facio-brachial focal seizures, secondarily generalized tonic-clonic seizures (GTCS), and centrotemporal epileptiform discharges.
    • Associated with oral and speech dyspraxia and cognitive impairment.
    • The speech disorder differs from that in Landau-Kleffner syndrome and epilepsy with continuous spike and wave during slow-wave sleep.

  • Demographic Data:

    • Studied in a family of nine affected individuals across three generations.
    • Patients in previous generations were less severely affected but also had neurological deficits, mainly oral and speech dyspraxia without evidence of dysarthria.

  • Clinical Manifestations:

    • Seizure Characteristics:
      • Nocturnal oro-facio-brachial focal seizures.
      • Secondarily generalized tonic-clonic seizures (GTCS).
      • Centrotemporal epileptiform discharges.
    • Neurological Deficits:
      • Prominent oral and speech dyspraxia.
      • Cognitive impairment.
      • In some cases, neurological deficits precede seizures.

  • Aetiology:

    • Autosomal dominant inheritance.
    • Clinical anticipation observed in seizure disorder, oral and speech dyspraxia, and cognitive dysfunction.
    • Genetic mechanism could involve expansion of an unstable triplet repeat.

  • Prognosis:

    • The condition shows clinical anticipation, meaning symptoms may worsen or appear earlier in successive generations.
    • Permanent neurological deficits make it distinct from benign rolandic epilepsy.

  • Clinical Significance:

    • Resembles benign rolandic epilepsy in some electroclinical features but differs due to permanent neurological deficits and anticipation.
    • Molecular studies on this syndrome may help identify a gene for benign rolandic epilepsy, where anticipation does not occur and the mode of inheritance is uncertain.

  • Management:

    • Specific management strategies not detailed; implications for treatment and genetic counseling need further research.

Focal Epilepsy with Pericentral Spikes

  • Overview:

    • Based on the study of a family with a variety of seizure types.
    • Seizure types include hemiclonic, hemitonic, generalized tonic-clonic seizures (GTCS), simple focal (stereotyped episodes of epigastric pain), and complex focal seizures with temporal lobe semiology.
    • The syndrome is benign, requiring no treatment or responding well to a single antiepileptic drug (AED).

  • Demographic Data:

    • Seizure onset typically occurs in the first or second decades of life.
    • Seizures can persist up to 71 years of age.
    • EEG changes have been documented up to the age of 30 years.

  • Clinical Manifestations:

    • Seizure Types:
      • Hemiclonic
      • Hemitonic
      • Generalized tonic-clonic seizures (GTCS)
      • Simple focal seizures (stereotyped episodes of epigastric pain)
      • Complex focal seizures consistent with temporal lobe semiology
    • EEG Abnormalities:
      • Characteristic spikes or sharp waves in the pericentral region:
        • Centroparietal
        • Centrofrontal
        • Centrotemporal
    • Variability:
      • The syndrome may be overlooked due to variability in penetrance and seizure types among affected family members.

  • Aetiology:

    • Evidence for linkage to chromosome 4p15.

  • Prognosis:

    • The syndrome is benign.
    • Seizures are either self-limiting or respond well to a single AED.

  • Management:

    • Treatment is often not required.
    • When needed, seizures respond well to a single AED.
Cite this: ICNApedia contributors.Familial (Autosomal Dominant) Focal Epilepsies. ICNApedia, The Child Neurology Knowledge Environment. 28 June 2024. Available at: https://icnapedia.org/knowledgebase/articles/familial-autosomal-dominant-focal-epilepsies Accessed  28 June 2024. 

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