POLG1 mutations cause a syndromic epilepsy with occipital lobe predilection

doi:10.1093/brain/awn007

Brain Advance Access originally published online on January 30, 2008
Brain 2008 131(3):818-828; doi:10.1093/brain/awn007

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POLG1 mutations cause a syndromic epilepsy with occipital lobe predilection

Bernt A. Engelsen¹^,2, Charalampos Tzoulis², Bjørn Karlsen², Atle Lillebø², Liv M. Lægreid⁴, Jan Aasly⁵, Massimo Zeviani³ and Laurence A. Bindoff¹^,2

¹Institute of Clinical Medicine, University of Bergen, ²Department of Neurology, Haukeland University Hospital, Bergen, Norway, ³Unit of Molecular Neurogenetics Pierfranco and Luisa Mariana Center for the Study of Children's Mitochondrial Disorders, National Neurological Institute "C.Besta", via Temolo 4, 20133 Milan, Italy, ⁴Department of Paediatrics, Haukeland University Hospital, Bergen and ⁵St Olav's Hospital, Trondheim, Norway

Correspondence to: Bernt A. Engelsen and Laurence Bindoff, Department of Neurology, Haukeland University Hospital, Helse-Bergen, HF. N-5021 Bergen, Norway E-mail: bernt.engelsen{at}helse-bergen.no, laurence.bindoff{at}helse-bergen.no

The epileptic semiology of 19 patients (from 15 families) withmitochondrial disease due to mutations in the POLG1 gene ispresented. The patients were either homozygous for the 1399G> A (p.A467T) or 2243G > C (p.W748S) mutations or compoundheterozygotes for these two mutations. While the clinical featureshave been reviewed, detailed analysis of their epilepsy is presentedfor the first time. Irrespective of genotype, patients developedan epileptic syndrome with initial features of occipital lobeepilepsy. Occipital seizure phenomena included flickering colouredlight, sometimes persisting for weeks, months or even years,ictal visual loss, horizontal/vertical nystagmus or oculoclonus,dysmorphopsia, micro-/macropsia and palinopsia. Most patientsdeveloped simple partial seizure phenomena with motor symptomssuggesting frontal lobe seizure initiation or spread. Simpleand complex partial seizures, clonic- and/or myoclonic seizureswith epilepsia partialis continua and frequent convulsive statusepilepticus were observed in this syndrome that appears to bea symptomatic and secondary generalized or multifocal epilepsywith focal occipital predilection. The mean age of seizure presentationwas 18.4 years (6–58 years). All patients developed statusepilepticus and 11 patient deaths were, all related to prolongedconvulsive status epilepticus, including two with liver failureapparently precipitated by treatment with sodium valproate.

Key Words: epilepsy; POLG; mitochondrial disease; occipital lobe; status epilepticus

Abbreviations: SE, status epilepticus; C-/NC, convulsive/non-convulsive; SPS, simple partial seizure; CPS, complex partial seizure; PLEDS, periodic lateralized epileptic discharges; sGTC, secondary generalized tonic–clonic seizures; EPC, epilepsia partialis continua

Received September 27, 2007. Revised January 4, 2008. Accepted January 8, 2008.

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