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Your search keyword '"Di Francesco, J. C."' showing total 6 results
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6 results on '"Di Francesco, J. C."'

1. Effectiveness of perampanel as the only add‐on: Retrospective, multicenter, observational real‐life study on epilepsy patients

Author

Gasparini S., Ferlazzo E., Neri S., Cianci V., Iudice A., Bisulli F., Bonanni P., Caggia E., D'Aniello A., Di Bonaventura C., Di Francesco J. C., Domina E., Dono F., Gambardella A., Marini C., Marrelli A., Matricardi S., Morano A., Paladin F., Renna R., Striano P., Pascarella A., Ascoli M., Aguglia U., PEROC Study Group, Gasparini S., Ferlazzo E., Neri S., Cianci V., Iudice A., Bisulli F., Bonanni P., Caggia E., D'Aniello A., Di Bonaventura C., Di Francesco J.C., Domina E., Dono F., Gambardella A., Marini C., Marrelli A., Matricardi S., Morano A., Paladin F., Renna R., Striano P., Pascarella A., Ascoli M., Aguglia U., and PEROC Study Group

Subjects
real-world, perampanel, Neurology, seizure freedom, early add-on, Neurology (clinical)
Abstract

Objective: Perampanel (PER) is indicated as adjunctive antiseizure medication (ASM) in adolescents and adults with epilepsy. Data from clinical trials show good efficacy and tolerability, while limited information is available on the routine clinical use of PER, especially when used as only add-on treatment. Methods: We performed an observational, retrospective, multicenter study on people with focal or generalized epilepsy aged >12 years, consecutively recruited from 52 Italian epilepsy centers. All patients received PER as the only add-on treatment to a background ASM according to standard clinical practice. Retention rate, seizure frequency, and adverse events were recorded at 3, 6, and 12months after PER introduction. Subanalyses by early or late use of PER and by concomitant ASM were also conducted. Results: Five hundred and three patients were included (age 36.5 ± 19.9 years). Eighty-one percent had focal epilepsy. Overall, the retention rate was very high in the whole group (89% at 12months) according with efficacy measures. No major differences were observed in the subanalyses, although patients who used PER as early add-on, as compared with late add-on, more often reached early seizure freedom at 3-month follow-up (66% vs 53%, P=.05). Treatment-emergent adverse events occurred in 25%, far less commonly than in PER randomized trials. Significance: This study confirms the good efficacy and safety of PER for focal or generalized epilepsy in real-life conditions. We provide robust data about its effectiveness as only add-on treatment even in patients with a long-standing history of epilepsy and previously treated with many ASMs.

Published
2022

3. Progressive epileptic encephalopathy associated with a novel HCN2 mutation

Author

Binda, A., Murano, C., Di Francesco, J. C., Castellotti, B., Milanesi, R., Ragona, F., Freri, E., Canafoglia, L., Franceschetti, S., Solazzi, R., tiziana granata, Gellera, C., Rivolta, I., Binda, A, Murano, C, DI FRANCESCO, J, Castellotti, B, Milanesi, R, Ragona, F, Freri, E, Canafoglia, L, Franceschetti, S, Solazzi, R, Granata, T, Gellera, C, and Rivolta, I

Subjects
epilepsy, HCN2, electrophysiology
Abstract

So far mutations in HCN2 gene, encoding for the hyperpolarization-activated cyclic nucleotide-gated channel 2, have been related to mild epileptic clinical phenotypes. In this study, a novel HCN2 mutation was found in a proband, now aged 7 years old, with a congenital encephalopathy characterized by drug resistant epilepsy, severe developmental delay, ataxia, dystonia and cerebral visual impairment. A convulsive status epilepticus at 5 months of age marked the onset of epilepsy. The HCN2 mutation affects an aminoacid located in the S6 transmembrane helix (p.Gly460Asp) and is carried in heterozygosis. To describe the functional consequences of the mutant channel, whole-cell patch-clamp experiments were performed in HEK293 cells expressing HCN2 wild type (WT) or p.Gly460Asp channel. A coexpression of the same amount of plasmid encoding for the wt or the mutant form of the channel mimed the heterozygous condition. A complete abolishment of the current was observed considering the mutant compared to the WT channel (-9.9±1.2 pA/pF, n=20 vs -31.2±8.4 pA/pF, n=44 respectively; p

5. Cerebral amyloid angiopathy-related inflammation: An emerging disease

Author

Floriano Girotti, J. C. Di Francesco, Alessandra Erbetta, M. Brioschi, Mario Savoiardo, Nicola Ticozzi, Andrea Falini, L. Brighina, Stefano Messina, G. Storchi, Vincenzo Silani, Carlo Ferrarese, Savoiardo, Mario, Erbetta, A., Di Francesco, J. C., Brioschi, M., Silani, V., Falini, A., Storchi, G., Brighina, L., Ferrarese, C., Ticozzi, N., Messina, S., Girotti, F., Savoiardo, M, Erbetta, A, DI FRANCESCO, J, Brioschi, M, Silani, V, Falini, A, Storchi, G, Brighina, L, Ferrarese, C, Ticozzi, N, Messina, S, and Girotti, F

Subjects
Apolipoprotein E, Pathology, medicine.medical_specialty, Radiology, Nuclear Medicine and Imaging, Amyloid, Inflammation, Disease, White matter, Microhemorrhage, Cortex (anatomy), Edema, mental disorders, medicine, Radiology, Nuclear Medicine and imaging, Cerebral amyloid angiopathy, business.industry, APOe, cerebral amyloid angiopathy-related inflammation , MRI, General Medicine, medicine.disease, medicine.anatomical_structure, Neurology (clinical), medicine.symptom, business, MRI
Abstract

Three elderly patients with, respectively: mild cognitive impairment, severe and progressive neurologic involvement, and focal neurologic deficit, were observed. MRI showed multiple areas of white matter edema, at times partially involving the cortex, in the first two patients, and a single area in the third. Treatment with steroids determined the disappearance of the lesions and clinical amelioration. The key to the diagnosis of cerebral amyloid angiopathy-related inflammation (CAA-ri) was the demonstration, with appropriate MRI sequences, of microbleeds consistent with cerebral amyloid angiopathy (CAA). This diagnosis was supported by genetic analysis of APOE with demonstration of ε4/ε4 genotype, found in about 80% of CAA patients who develop inflammatory changes. In the appropriate clinical setting, MRI demonstration of microbleeds supported by results of genetic analysis of APOE may strongly support the diagnosis of CAA-ri thus avoiding cerebral biopsy.

6. Cerebral amyloid angiopathy-related inflammation: an emerging disease.

Author

Savoiardo M, Erbetta A, Di Francesco JC, Brioschi M, Silani V, Falini A, Storchi G, Brighina L, Ferrarese C, Ticozzi N, Messina S, and Girotti F

Abstract

Three elderly patients with, respectively: mild cognitive impairment, severe and progressive neurologic involvement, and focal neurologic deficit, were observed. MRI showed multiple areas of white matter edema, at times partially involving the cortex, in the first two patients, and a single area in the third. Treatment with steroids determined the disappearance of the lesions and clinical amelioration. The key to the diagnosis of cerebral amyloid angiopathy-related inflammation (CAA-ri) was the demonstration, with appropriate MRI sequences, of microbleeds consistent with cerebral amyloid angiopathy (CAA). This diagnosis was supported by genetic analysis of APOE with demonstration of ε4/ε4 genotype, found in about 80% of CAA patients who develop inflammatory changes. In the appropriate clinical setting, MRI demonstration of microbleeds supported by results of genetic analysis of APOE may strongly support the diagnosis of CAA-ri thus avoiding cerebral biopsy.

Published
2011
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