Your search keyword '"Specchio, N."' showing total 10 results

1. West syndrome associated with 14q12 duplications harboring FOXG1

Author

Striano, P., primary, Paravidino, R., additional, Sicca, F., additional, Chiurazzi, P., additional, Gimelli, S., additional, Coppola, A., additional, Robbiano, A., additional, Traverso, M., additional, Pintaudi, M., additional, Giovannini, S., additional, Operto, F., additional, Vigliano, P., additional, Granata, T., additional, Coppola, G., additional, Romeo, A., additional, Specchio, N., additional, Giordano, L., additional, Osborne, L. R., additional, Gimelli, G., additional, Minetti, C., additional, and Zara, F., additional

Published

2011

2. Protocadherin 19 mutations in girls with infantile-onset epilepsy

Author

Marini, C., primary, Mei, D., additional, Parmeggiani, L., additional, Norci, V., additional, Calado, E., additional, Ferrari, A., additional, Moreira, A., additional, Pisano, T., additional, Specchio, N., additional, Vigevano, F., additional, Battaglia, D., additional, and Guerrini, R., additional

Published

2010

3. An open-label trial of levetiracetam in severe myoclonic epilepsy of infancy

Author

Striano, P., primary, Coppola, A., additional, Pezzella, M., additional, Ciampa, C., additional, Specchio, N., additional, Ragona, F., additional, Mancardi, M. M., additional, Gennaro, E., additional, Beccaria, F., additional, Capovilla, G., additional, Rasmini, P., additional, Besana, D., additional, Coppola, G. G., additional, Elia, M., additional, Granata, T., additional, Vecchi, M., additional, Vigevano, F., additional, Viri, M., additional, Gaggero, R., additional, Striano, S., additional, and Zara, F., additional

Published

2007

4. Resective surgery for epileptogenic dysembryoplastic neuroepithelial tumor in hemimegalencephaly.

Author

Specchio N, Kahane P, Pasquier B, Tassi L, and Guerrini R

Published

2005

5. Outcome of Epilepsy Surgery in MRI-Negative Patients Without Histopathologic Abnormalities in the Resected Tissue.

Author

Sanders MW, Van der Wolf I, Jansen FE, Aronica E, Helmstaedter C, Racz A, Surges R, Grote A, Becker AJ, Rheims S, Catenoix H, Duncan JS, De Tisi J, Jacques TS, Cross JH, Kalviainen R, Rauramaa T, Chassoux F, Devaux BC, Di Gennaro G, Esposito V, Bodi I, Honavar M, Bien CG, Cloppenborg T, Coras R, Hamer HM, Marusic P, Kalina A, Pieper T, Kudernatsch M, Hartlieb TS, Von Oertzen TJ, Aichholzer M, Dorfmuller G, Chipaux M, Noachtar S, Kaufmann E, Schulze-Bonhage A, Scheiwe CF, Özkara C, Grunwald T, Koenig K, Guerrini R, Barba C, Buccoliero AM, Giordano F, Rosenow F, Menzler K, Garbelli R, Deleo F, Krsek P, Straka B, Arzimanoglou AA, Toulouse J, Van Paesschen W, Theys T, Pimentel J, Loução De Amorim IM, Specchio N, De Palma L, Feucht M, Scholl T, Roessler K, Toledano Delgado R, Gil-Nagel A, Raicevic S, Ristic AJ, Schijns O, Beckervordersandforth J, San Antonio-Arce V, Rumia J, Blumcke I, and Braun KP

Subjects

Humans, Cohort Studies, Electroencephalography, Magnetic Resonance Imaging, Retrospective Studies, Seizures, Treatment Outcome, Epilepsies, Partial diagnostic imaging, Epilepsies, Partial surgery, Epilepsy diagnostic imaging, Epilepsy surgery, Epilepsy, Temporal Lobe surgery

Abstract

Background and Objective: Patients with presumed nonlesional focal epilepsy-based on either MRI or histopathologic findings-have a lower success rate of epilepsy surgery compared with lesional patients. In this study, we aimed to characterize a large group of patients with focal epilepsy who underwent epilepsy surgery despite a normal MRI and had no lesion on histopathology. Determinants of their postoperative seizure outcomes were further studied., Methods: We designed an observational multicenter cohort study of MRI-negative and histopathology-negative patients who were derived from the European Epilepsy Brain Bank and underwent epilepsy surgery between 2000 and 2012 in 34 epilepsy surgery centers within Europe. We collected data on clinical characteristics, presurgical assessment, including genetic testing, surgery characteristics, postoperative outcome, and treatment regimen., Results: Of the 217 included patients, 40% were seizure-free (Engel I) 2 years after surgery and one-third of patients remained seizure-free after 5 years. Temporal lobe surgery (adjusted odds ratio [AOR]: 2.62; 95% CI 1.19-5.76), shorter epilepsy duration (AOR for duration: 0.94; 95% CI 0.89-0.99), and completely normal histopathologic findings-versus nonspecific reactive gliosis-(AOR: 4.69; 95% CI 1.79-11.27) were significantly associated with favorable seizure outcome at 2 years after surgery. Of patients who underwent invasive monitoring, only 35% reached seizure freedom at 2 years. Patients with parietal lobe resections had lowest seizure freedom rates (12.5%). Among temporal lobe surgery patients, there was a trend toward favorable outcome if hippocampectomy was part of the resection strategy (OR: 2.94; 95% CI 0.98-8.80). Genetic testing was only sporadically performed., Discussion: This study shows that seizure freedom can be reached in 40% of nonlesional patients with both normal MRI and histopathology findings. In particular, nonlesional temporal lobe epilepsy should be regarded as a relatively favorable group, with almost half of patients achieving seizure freedom at 2 years after surgery-even more if the hippocampus is resected-compared with only 1 in 5 nonlesional patients who underwent extratemporal surgery. Patients with an electroclinically identified focus, who are nonlesional, will be a promising group for advanced molecular-genetic analysis of brain tissue specimens to identify new brain somatic epilepsy genes or epilepsy-associated molecular pathways.

Published

2024

6. Movement Disorders in Patients With Genetic Developmental and Epileptic Encephalopathies.

Author

van der Veen S, Tse GTW, Ferretti A, Garone G, Post B, Specchio N, Fung VSC, Trivisano M, and Scheffer IE

Subjects

Humans, Infant, Child, Preschool, Child, Adolescent, Young Adult, Adult, Infant, Newborn, Tremor, Ataxia, Dystonia genetics, Movement Disorders genetics, Dystonic Disorders genetics, Brain Diseases genetics

Abstract

Background and Objectives: Movement disorders (MDs) are underrecognized in the developmental and epileptic encephalopathies (DEEs). There are now more than 800 genes implicated in causing the DEEs; relatively few of these rare genetic diseases are known to be associated with MDs. We identified patients with genetic DEEs who had MDs, classified the nature of their MDs, and asked whether specific patterns correlated with the underlying mechanism., Methods: We classified the type of MDs associated with specific genetic DEEs in a large international cohort of patients and analyzed whether specific patterns of MDs reflected the underlying biological dysfunction., Results: Our cohort comprised 77 patients with a genetic DEE with a median age of 9 (range 1-38) years. Stereotypies (37/77, 48%) and dystonia (34/77, 44%) were the most frequent MDs, followed by chorea (18/77, 23%), myoclonus (14/77, 18%), ataxia (9/77, 12%), tremor (7/77, 9%), and hypokinesia (6/77, 8%). In 47% of patients, a combination of MDs was seen. The MDs were first observed at a median age of 18 months (range day 2-35 years). Dystonia was more likely to be observed in nonambulatory patients, while ataxia was less likely. In 46% of patients, therapy was initiated with medication (34/77, 44%), deep brain stimulation (1/77, 1%), or intrathecal baclofen (1/77, 1%). We found that patients with channelopathies or synaptic vesicle trafficking defects were more likely to experience dystonia; whereas, stereotypies were most frequent in individuals with transcriptional defects., Discussion: MDs are often underrecognized in patients with genetic DEEs, but recognition is critical for the management of these complex neurologic diseases. Distinguishing MDs from epileptic seizures is important in tailoring patient treatment. Understanding which MDs occur with different biological mechanisms will inform early diagnosis and management., (© 2023 American Academy of Neurology.)

Published

2023

7. The phenotype of SCN8A developmental and epileptic encephalopathy.

Author

Gardella E, Marini C, Trivisano M, Fitzgerald MP, Alber M, Howell KB, Darra F, Siliquini S, Bölsterli BK, Masnada S, Pichiecchio A, Johannesen KM, Jepsen B, Fontana E, Anibaldi G, Russo S, Cogliati F, Montomoli M, Specchio N, Rubboli G, Veggiotti P, Beniczky S, Wolff M, Helbig I, Vigevano F, Scheffer IE, Guerrini R, and Møller RS

Subjects

Adolescent, Child, Child, Preschool, Developmental Disabilities complications, Developmental Disabilities genetics, Electroencephalography, Female, Humans, Infant, Male, Mutation, NAV1.6 Voltage-Gated Sodium Channel genetics, Spasms, Infantile complications, Spasms, Infantile genetics, Young Adult, Developmental Disabilities diagnosis, Spasms, Infantile diagnosis

Abstract

Objective: To delineate the electroclinical features of SCN8A infantile developmental and epileptic encephalopathy (EIEE13, OMIM #614558)., Methods: Twenty-two patients, aged 19 months to 22 years, underwent electroclinical assessment., Results: Sixteen of 22 patients had mildly delayed development since birth. Drug-resistant epilepsy started at a median age of 4 months, followed by developmental slowing, pyramidal/extrapyramidal signs (22/22), movement disorders (12/22), cortical blindness (17/22), sialorrhea, and severe gastrointestinal symptoms (15/22), worsening during early childhood and plateauing at age 5 to 9 years. Death occurred in 4 children, following extreme neurologic deterioration, at 22 months to 5.5 years. Nonconvulsive status epilepticus recurred in 14 of 22 patients. The most effective antiepileptic drugs were oxcarbazepine, carbamazepine, phenytoin, and benzodiazepines. EEG showed background deterioration, epileptiform abnormalities with a temporo-occipital predominance, and posterior delta/beta activity correlating with visual impairment. Video-EEG documented focal seizures (FS) (22/22), spasm-like episodes (8/22), cortical myoclonus (8/22), and myoclonic absences (1/22). FS typically clustered and were prolonged (<20 minutes) with (1) cyanosis, hypomotor, and vegetative semiology, sometimes unnoticed, followed by (2) tonic-vibratory and (3) (hemi)-clonic manifestations ± evolution to a bilateral tonic-clonic seizure. FS had posterior-temporal/occipital onset, slowly spreading and sometimes migrating between hemispheres. Brain MRI showed progressive parenchymal atrophy and restriction of the optic radiations., Conclusions: SCN8A developmental and epileptic encephalopathy has strikingly consistent electroclinical features, suggesting a global progressive brain dysfunction primarily affecting the temporo-occipital regions. Both uncontrolled epilepsy and developmental compromise contribute to the profound impairment (increasing risk of death) during early childhood, but stabilization occurs in late childhood., (© 2018 American Academy of Neurology.)

Published

2018

8. Clinical and genetic factors predicting Dravet syndrome in infants with SCN1A mutations.

Author

Cetica V, Chiari S, Mei D, Parrini E, Grisotto L, Marini C, Pucatti D, Ferrari A, Sicca F, Specchio N, Trivisano M, Battaglia D, Contaldo I, Zamponi N, Petrelli C, Granata T, Ragona F, Avanzini G, and Guerrini R

Subjects

Adolescent, Adult, Age of Onset, Aged, Aged, 80 and over, Child, Child, Preschool, Electroencephalography, Epilepsies, Myoclonic diagnosis, Epilepsies, Myoclonic physiopathology, Female, Genetic Association Studies, Humans, Infant, Longitudinal Studies, Male, Middle Aged, ROC Curve, Statistics, Nonparametric, Young Adult, Epilepsies, Myoclonic genetics, Mutation genetics, NAV1.1 Voltage-Gated Sodium Channel genetics

Abstract

Objective: To explore the prognostic value of initial clinical and mutational findings in infants with SCN1A mutations., Methods: Combining sex, age/fever at first seizure, family history of epilepsy, EEG, and mutation type, we analyzed the accuracy of significant associations in predicting Dravet syndrome vs milder outcomes in 182 mutation carriers ascertained after seizure onset. To assess the diagnostic accuracy of all parameters, we calculated sensitivity, specificity, receiver operating characteristic (ROC) curves, diagnostic odds ratios, and positive and negative predictive values and the accuracy of combined information. We also included in the study demographic and mutational data of the healthy relatives of mutation carrier patients., Results: Ninety-seven individuals (48.5%) had Dravet syndrome, 49 (23.8%) had generalized/genetic epilepsy with febrile seizures plus, 30 (14.8%) had febrile seizures, 6 (3.5%) had focal epilepsy, and 18 (8.9%) were healthy relatives. The association study indicated that age at first seizure and frameshift mutations were associated with Dravet syndrome. The risk of Dravet syndrome was 85% in the 0- to 6-month group, 51% in the 6- to 12-month range, and 0% after the 12th month. ROC analysis identified onset within the sixth month as the diagnostic cutoff for progression to Dravet syndrome (sensitivity = 83.3%, specificity = 76.6%)., Conclusions: In individuals with SCN1A mutations, age at seizure onset appears to predict outcome better than mutation type. Because outcome is not predetermined by genetic factors only, early recognition and treatment that mitigates prolonged/repeated seizures in the first year of life might also limit the progression to epileptic encephalopathy., (© 2017 American Academy of Neurology.)

Published

2017

9. Claustrum damage and refractory status epilepticus following febrile illness.

Author

Meletti S, Slonkova J, Mareckova I, Monti G, Specchio N, Hon P, Giovannini G, Marcian V, Chiari A, Krupa P, Pietrafusa N, Berankova D, and Bar M

Subjects

Adult, Anticonvulsants therapeutic use, Brain Injuries, Electroencephalography methods, Female, Humans, Magnetic Resonance Imaging methods, Male, Retrospective Studies, Seizures drug therapy, Status Epilepticus drug therapy, Young Adult, Basal Ganglia pathology, Seizures pathology, Status Epilepticus pathology

Abstract

Objective: To characterize the clinical, EEG, and brain imaging findings in an adult case series of patients with de novo refractory status epilepticus (SE) occurring after a febrile illness., Methods: A retrospective study (2010-2013) was undertaken with the following inclusion criteria: (1) previously healthy adults with refractory SE; (2) seizure onset 0-21 days after a febrile illness; (3) lacking evidence of infectious agents in CSF; (4) no history of seizures (febrile or afebrile) or previous or concomitant neurologic disorder., Results: Among 155 refractory SE cases observed in the study period, 6 patients (17-35 years old) fulfilled the inclusion criteria. Confusion and stupor were the most common symptoms at disease onset, followed after a few days by acute repeated seizures that were uncountable in all but one. Seizures consisted of focal motor/myoclonic phenomena with subsequent generalization. Antiepileptic drugs failed in every patient to control seizures, with all participants requiring intensive care unit admission. Barbiturate coma with burst-suppression pattern was applied in 4 out of 6 patients for 5-14 days. One participant died in the acute phase. In each patient, we observed a reversible bilateral claustrum MRI hyperintensity on T2-weighted sequences, without restricted diffusion, time-related with SE. All patients had negative multiple neural antibodies testing. Four out of 5 surviving patients developed chronic epilepsy., Conclusions: This is a hypothesis-generating study of a preliminary nature supporting the role of the claustrum in postfebrile de novo SE; future prospective studies are needed to delineate the specificity of this condition, its pathogenesis, and the etiology., (© 2015 American Academy of Neurology.)

Published

2015

10. The phenotypic spectrum of SCN8A encephalopathy.

Author

Larsen J, Carvill GL, Gardella E, Kluger G, Schmiedel G, Barisic N, Depienne C, Brilstra E, Mang Y, Nielsen JE, Kirkpatrick M, Goudie D, Goldman R, Jähn JA, Jepsen B, Gill D, Döcker M, Biskup S, McMahon JM, Koeleman B, Harris M, Braun K, de Kovel CG, Marini C, Specchio N, Djémié T, Weckhuysen S, Tommerup N, Troncoso M, Troncoso L, Bevot A, Wolff M, Hjalgrim H, Guerrini R, Scheffer IE, Mefford HC, and Møller RS

Subjects

Adolescent, Brain Diseases diagnosis, Brain Diseases physiopathology, Child, Child, Preschool, Electroencephalography methods, Epilepsy diagnosis, Epilepsy physiopathology, Female, Follow-Up Studies, Humans, Infant, Internationality, Male, Brain Diseases genetics, Epilepsy genetics, Mutation genetics, NAV1.6 Voltage-Gated Sodium Channel genetics, Phenotype

Abstract

Objective: SCN8A encodes the sodium channel voltage-gated α8-subunit (Nav1.6). SCN8A mutations have recently been associated with epilepsy and neurodevelopmental disorders. We aimed to delineate the phenotype associated with SCN8A mutations., Methods: We used high-throughput sequence analysis of the SCN8A gene in 683 patients with a range of epileptic encephalopathies. In addition, we ascertained cases with SCN8A mutations from other centers. A detailed clinical history was obtained together with a review of EEG and imaging data., Results: Seventeen patients with de novo heterozygous mutations of SCN8A were studied. Seizure onset occurred at a mean age of 5 months (range: 1 day to 18 months); in general, seizures were not triggered by fever. Fifteen of 17 patients had multiple seizure types including focal, tonic, clonic, myoclonic and absence seizures, and epileptic spasms; seizures were refractory to antiepileptic therapy. Development was normal in 12 patients and slowed after seizure onset, often with regression; 5 patients had delayed development from birth. All patients developed intellectual disability, ranging from mild to severe. Motor manifestations were prominent including hypotonia, dystonia, hyperreflexia, and ataxia. EEG findings comprised moderate to severe background slowing with focal or multifocal epileptiform discharges., Conclusion: SCN8A encephalopathy presents in infancy with multiple seizure types including focal seizures and spasms in some cases. Outcome is often poor and includes hypotonia and movement disorders. The majority of mutations arise de novo, although we observed a single case of somatic mosaicism in an unaffected parent., (© 2015 American Academy of Neurology.)

Published

2015