1 / 71

Syndromic Diagnosis and Interictal Correlation of Epilepsies

Syndromic Diagnosis and Interictal Correlation of Epilepsies. Dr.Ashraf.V.V Consultant Neurologist MIMS Hospital, Calicut. Electro-clinical Syndrome. Group of clinical entities that are reliably identified by a cluster of electro-clinical and developmental characteristics

cullen-newman
Download Presentation

Syndromic Diagnosis and Interictal Correlation of Epilepsies

An Image/Link below is provided (as is) to download presentation Download Policy: Content on the Website is provided to you AS IS for your information and personal use and may not be sold / licensed / shared on other websites without getting consent from its author. Content is provided to you AS IS for your information and personal use only. Download presentation by click this link. While downloading, if for some reason you are not able to download a presentation, the publisher may have deleted the file from their server. During download, if you can't get a presentation, the file might be deleted by the publisher.

E N D

Presentation Transcript

  1. Syndromic Diagnosis and Interictal Correlation of Epilepsies Dr.Ashraf.V.V Consultant Neurologist MIMS Hospital, Calicut

  2. Electro-clinical Syndrome • Group of clinical entities that are reliably identified by a cluster of electro-clinical and developmental characteristics • Largely genetic in origin • Tend to have a strong relationship to developmental aspects of brain ILAE Commission 2009

  3. Concept of Epileptic Syndromes • Factors taken into consideration include • Seizure type(s) • Age of Onset • Precipitating factors • Severity, Chronicity • Diurnal/circadian cycling • Etiology: genetics, structural pathology • Associated neurological problems • Interictal EEG

  4. Advantages of a syndromic diagnosis Provide information about • Age of onset • Etiology • Seizure type • Precipitating factors • Chronicity • Prognosis • Choice of treatment

  5. Epileptic Encephalopathy • Electro-clinical syndrome associated with a very high probability of encephalopathic features that present or worsen after the onset of epilepsy • Pharmaco-resistant

  6. Neonatal Epileptic syndromes • Early Myoclonic encephalopathy • Ohtahara syndrome • Benign familial neonatal seizures

  7. Early Myoclonic Encephalopathy(Aicardi et al 1978) • Onset: first weeks of life • Erratic, focal, rarely generalized myoclonic and clonic seizures • High incidence of consanguinity • Sometimes IEMs: (NKHG) • EEG: Burst- Suppression Pattern, persists for months; awake & sleep • Intractable to therapy - seizure pattern may change over time • Severe disability; early death

  8. 3 months later

  9. Early Infantile Epileptic Encephalopathy (Ohtahara 1976) • Onset in the first weeks of life • Characteristic repetitive ‘tonic spasms’ - focal or generalized • Commonly associated with structural brain abnormalities • EEG burst suppression pattern, > in sleep, evolves to hypsarrythmia • Intractable to AEDs • Neurological outcome is very poor, early death • Evolves to WS, LGS

  10. Fp1-F3 F3 –C3 C3 – P3 P3 – O1 Fp2 F4 F4 – C4 C4 – P4 P4 – O2 Fp1 –F7 F7 – T3 T3 – T5 T5 – O1 Fp2 F8 F8 – T4 T4 – T6 T6 – O2 EKG

  11. Benign familial neonatal Seizures • Second or third day of life • Repetitive isolated seizures • Autosomal dominant • 10-15% develop epilepsy later • No psychomotor deficit • EEG: Non specific, focal abnormalities

  12. Electro-clinical syndromes of Infancy • West syndrome • Febrile seizures plus • Dravet syndrome • Migrating partial seizures of infancy • Myoclonic epilepsy in infancy • Myoclonic encephalopathy in nonprogressive disorders • Benign familial infantile seizures

  13. WEST SYNDROME : INFANTILE (EPILEPTIC) SPASMS • Myoclonic < Spasms< Tonic • Flexor , Extensor, Flexor-extensor • Subtle spasm • Asymmetrical spasm in symptomatic • Onset 3-12 m (4 months); till 2 yrs • Occipital lesions----early onset Frontal lesions -----later onset

  14. West Syndrome • Symptomatic , Cryptogenic, Idiopathic • Symptomatic- cortical malformations, HIE, tuberous sclerosis,infections, genetic and chromosomal abnormalities etc • Focal lesions ++ • Autistic regression / visual agnosia • Evolution LGS / partial seizures

  15. Inter-ictal Hypsarrthymmia (50-60%): Chaotic background with high amplitude delta,asynchronous multifocal spikes, polyspikes and electrodecremental activity Awake

  16. Hypsarrhythmia with focal slowing (Left temporo-occipital FCD )

  17. Spasms & hypsarrhythmia resolve by 2y Evolve to focal seizures (R occipital lesion)

  18. Ictal- Generalised sharpwaves/slow waves with attenuation

  19. WHEN FEBRILE SEIZURES ARE NOT FEBRILE SEIZURES • GEFS + (Gen. Epilepsy febrile seizures plus) • Common under-recognised disorder • Autosomal dominant with high penetrance • Typical FS, FS + lasting longer, Afebrile GTCs most common • Occasionally absence, myoclonic, atonic • Focal seizures of frontal or temporal lobe in origin • Dravet’s syndrome overlap • Remits in adolescence 80% • Sodium channelopathy

  20. Dravet’s syndrome (SMEI) • 1st year febrile / afebrile unilateral / GTCs; status epilepticus • Later myoclonus, atypical absence, complex focal • Resistant to AEDs • Cognitive regression, ataxia 2nd year • FH + 25-30% • Severe idiopathic generalised epilepsy of infancy (SIGEI) with GTCs: No myoclonus

  21. EEGs normal ; later generalized epileptic photosensitivity • Consider this syndrome when febrile / illness provoked seizures start in infancy and EEG is persistently NORMAL

  22. EM-AS GEFS + SCN1A mutations DRAVETs SIGEI

  23. Malignant migrating partial epilepsy of Infancy • Epileptic encephalopathy • Mean age 3 months • Continuous multifocal seizures arising independently from multiple regions • Psychomotor deterioration • Seizure control is exceptional

  24. Malignant migrating partial epilepsy of infancy Migrating seizures of infantile

  25. Migrating seizures of infantile

  26. Childhood epilepsy syndromes • Benign epilepsy with centrotemporal spikes • Early onset Benign childhood occipital epilepsy (Panayiotopoulos Syndrome) • Late onset childhood occipital epilepsy (Gastaut type) • Epileptic encephalopathy with CSWS • Landau-Kleffner syndrome • Lennox-Gastaut syndrome • Autosomal dominant nocturnal frontal lobe epilepsy • Childhood Absence epilepsy • Epilepsy with myoclonic absence

  27. BECTS[Benign Rolandic Epilepsy] • Most common partial epilepsy in childhood • Onset 2-14 years; ¾ 7-10 yrs • Seizure frequency- • 10-20% have a single seizure • 20% have frequent seizures • < 2% have seizures into adulthood • “No other” neurological issues

  28. Ictal Semiology Focalfacial sensorimotor 70% nocturnal 60% retained awareness Lasts 1-2 min Sec. Generalized- 30-50% Oro-pharyngo-laryngeal Hyper salivation Speech arrest Clonic upperlimb

  29. Panayiotopoulos Syndrome Tonic eye deviation 70% nocturnal Peak- 4 to 5 years Lasts longer; 44% > 30 min EEG focus-commonly occipital, variability ++ N, R, Vomiting Pallor + other autonomic Ictal syncope

  30. Idiopathic childhood occipital epilepsy of Gastaut • Mean age : 8 years • Elementary visual hallucinations • Ictal blindness • Deviation of eyes • Severe headache • EEG shows occipital paroxysms, often demonstrating fixation-off sensitivity

  31. Epileptic Encephalopathy of Late Childhood LKS CSWS A spectrum of diseases Landau- Kleffner syndrome CSWS Syndrome Gradual cognitive/behavior deterioration Acquired language impairment Seizures Dramatic activation of epileptiform abnormalities in slow wave sleep

  32. Landau Kleffner Syndrome • Our son was normal in every way until the age of 2 years. At first he seemed to be losing his hearing but not for environmental sounds. We thought that he was going deaf, but the hearing test was normal… When he was 3 years old he didn’t say anything for over a month. He improved for a few months and then he had a minor seizure • From the internet description by a mother

  33. LKS CSWS 80% Spikes Temporal Seizures 75% Symptomatic rare Verbal auditory agnosia Behavioural deficit common 50% reach near normal life Epilepsy with CSWS CSWS 100% Frontal spikes Seizures -100% One third symptomatic Expressive aphasia Nearly all One-quarter reach normal LKS Vs Epilepsy with CSWS

  34. Fp1-F3 F3 –C3 C3 – P3 P3 – O1 Fp2 F4 F4 – C4 C4 – P4 P4 – O2 Fp1 –F7 F7 – T3 T3 – T5 T5 – O1 Fp2 F8 F8 – T4 T4 – T6 T6 – O2 EKG

  35. Lennox Gastaut Syndrome • Polymorphic seizures Tonic Seizures - Commonest Atypical absences – 2/3rd of patients Atonic seizures (Drop attacks) Myoclonic jerks • Cognitive and behavioural abnormalities • EEGSlow spike and wave, Paroxysms of fast activity

  36. Lennox-Gastaut Syndrome • Peak age 3-5 years • Symptomatic form most common • One third idiopathic • No genetic predisposition • Half of the West syndrome and others progress to LGS • Poor prognosis

  37. EVOLUTION OF SYNDROMES OTAHARA’S (neonate) WEST (infant) LENNOX GASTAUT (toddler)

  38. D 15 infant refractory tonic / partial seizures; BH N MRI N / Metabolic N EE with suppression – burst (OTOHARA’s )

  39. Epileptic spasms a few months later HYPSARRYTHMIA MODIFIED BY SLEEP

  40. 2.5 y; MR, Tonic seizures in sleep; Drop attacks with injuries; Episodes of atypical absence status & regression SLOW SPIKE WAVE-LGS

More Related