PIGN encephalopathy: Characterizing the epileptology.

Allan Bayat,Patrick Carney,Pasquelena De Nittis,Joost Nicolai,Caroline Maxton,Roberta Vittorini,Jennifer Norman,Rikke S Møller,Sarah Weckhuysen,Aleksandra Jezela‐Stanek,Patrick Edery,Annapurna Poduri,Barbara Oleksy,Eleina England,Ewa Pronicka,Pasquale Striano,Sonja Walsh,Berten Ceulemans,Boris Keren,Fernando Santos‐Simarro,Eva Maria Christina Schwaibold,Barbara Weissman,Ingrid E Scheffer,Michael S Hildebrand,Manuela Pendziwiat,Marius Kuhn,Iwona Terczyńska,Charlotte Peinhardt,Sandra Monfort,Andreas Tzschach,Alexej Knaus,Johannes R Lemke,Hong Li,Patrick Van Bogaert,Sophie Calvert,Kerstin Alt,Janice Cousin,Magali Gorce,Alexandre Reymond,Vincent Des Portes,Katja Kloth,Elisa Biamino,Carmen Orellana,Giuseppe Merla,Annette Bley,Lynette G Sadleir,Blanca Gener,Gerhard Kluger,Hanna Mierzewska,Julien Thévenon ,Heather C Mefford ,Delphine Héron ,Heather E Olson ,Mónica Roselló ,Pierre-Simon Jouk ,Guillem De Valles-Ibáñez ,Constance T R M Stumpel ,Gina L O’grady ,Jeremy L Freeman ,Suzanne L Davis ,Francisco Martı́nez ,Elżbieta Szczepanik ,Gaëtan Lesca ,Alison M Muir ,Carlos R Ferreira ,Alexander P.a Stegmann ,Alfonso Caro-Llopis ,Lynne A Wolfe ,Laura Orec

doi:10.1111/epi.17173

Abstract

Epilepsy is common in patients with PIGN diseases due to biallelic variants; however, limited epilepsy phenotyping data have been reported. We describe the epileptology of PIGN encephalopathy. We recruited patients with epilepsy due to biallelic PIGN variants and obtained clinical data regarding age at seizure onset/offset and semiology, development, medical history, examination, electroencephalogram, neuroimaging, and treatment. Seizure and epilepsy types were classified. Twenty six patients (13 female) from 26 families were identified, with mean age 7years (range = 1month to 21years; three deceased). Abnormal development at seizure onset was present in 25 of 26. Developmental outcome was most frequently profound (14/26) or severe (11/26). Patients presented with focal motor (12/26), unknown onset motor (5/26), focal impaired awareness (1/26), absence (2/26), myoclonic (2/26), myoclonic-atonic (1/26), and generalized tonic-clonic (2/26) seizures. Twenty of 26 were classified as developmental and epileptic encephalopathy (DEE): 55% (11/20) focal DEE, 30% (6/20) generalized DEE, and 15% (3/20) combined DEE. Six had intellectual disability and epilepsy (ID+E): twogeneralized and four focal epilepsy. Mean age at seizure onset was 13months (birth to 10years), with a lower mean onset in DEE (7months) compared with ID+E (33months). Patients with DEE had drug-resistant epilepsy, compared to 4/6 ID+E patients, who were seizure-free. Hyperkinetic movement disorder occurred in 13 of 26 patients. Twenty-seven of 34 variants were novel. Variants were truncating (n = 7), intronic and predicted to affect splicing (n = 7), and missense or inframe indels (n = 20, of which 11 were predicted to affect splicing). Seven variants were recurrent, including p.Leu311Trp in 10 unrelated patients, nine with generalized seizures, accounting for nine of the 11 patients in this cohort with generalized seizures. PIGN encephalopathy is a complex autosomal recessive disorder associated with a wide spectrum of epilepsy phenotypes, typically with substantial profound to severe developmental impairment.

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