Through this section, we share the opportunity of collaborative clinical research calls such as natural history studies.
The main aim of this initiative, supported by the EpiCARE network, is to facilitate recruitment of cohorts of patients across epilepsy centres.
You will find the submission template here. Please follow the instructions in the template and send it back to Valentina De Giorgis.
Please find below the list of current calls. Click on the + sign for more information and contact details.
Background and Rationale
Phelan-McDermid syndrome (PMS), caused by deletions or pathogenic variants involving SHANK3, is a rare neurodevelopmental disorder characterized by global developmental delay, intellectual disability, autism spectrum disorder, and a variable risk of epilepsy. The pooled prevalence of seizures in PMS, is approximately 32% (Holder & Quach, 2016), while lifetime prevalence at adult age may reach up to 60% (de Coo 2023). Seizure onset can occur at any age, with no clearly identified developmental period at higher risk. Both febrile and non-febrile seizures have been reported, with atypical absences being the most frequently described seizure type.
EEG abnormalities are common in PMS; deletion of SHAK3 increases the risk of all types of seizures, irrespective the size of deletion (de Coo 2023). Neither seizures nor EEG abnormalities per se have been consistently linked to developmental regression. To date, no clinical, electrophysiological, or biological markers have been identified to predict regression or psychiatric deterioration in individuals with PMS (Kohlenberg et al., 2020). Furthermore, no antiepileptic drug has demonstrated clear superiority in the treatment of epilepsy in PMS, supporting a multifactorial model in which SHANK3 haploinsufficiency may alter excitation–inhibition balance or energy utilization in specific brain circuits, while additional genetic or environmental factors are likely required to precipitate seizures (de Coo 2023).
SWAS and PMS: a Potentially Under-recognized Association
Several monogenic causes of SWAS have been described, most notably GRIN2A, as well as SCN2A, FRRS1L, CNKSR2, CDKL5, and recurrent CNVs such as dup15q. In contrast, the association between SWAS and SHANK3 alterations remains largely unexplored, with only one isolated report describing SWAS in an individuals with PMS (deletion).
Recent clinical experience at the Mondino Hospital with a patient affected by PMS and SWAS, presenting with concomitant psychomotor regression and showing a marked and sustained response to intravenous steroid therapy, raises the possibility that SWAS in PMS may be underdiagnosed or misinterpreted. Subsequently, other Italian centers have shared similar clinical experiences, further supporting this hypothesis. Importantly, current treatment guidelines for PMS-associated epilepsy do not specifically address SWAS, nor do they recommend steroid therapy in this context.
Study objectives
The primary aim of this multicenter descriptive study is to investigate the prevalence of SWAS in Phelan-McDermid syndrome.
Secondary objectives include:
Call for Collaboration
We invite colleagues to contribute cases of individuals with genetically confirmed Phelan-McDermid syndrome who have demonstrated SWAS. By pooling clinical, EEG, genetic, and treatment response data, this study aims to improve recognition of SWAS in PMS, refine its clinical characterization, and generate preliminary evidence to inform future diagnostic and therapeutic recommendations.
Call published on 12 February 2026.
This study aims to investigate plasma amino-acid profiles in patients with TSC-related epilepsy treated with a ketogenic diet (KD), compared with age-matched non-TSC epilepsy controls. Using retrospective clinical and laboratory data, the project will assess metabolic alterations, with a particular focus on amino acids involved in mTOR signaling (including branched-chain amino acids). Where available, paired measurements before and after KD initiation will be analyzed to explore treatment-related metabolic changes. The study will also investigate associations between metabolic profiles, seizure burden, and clinical outcomes, and explore potential biomarkers of treatment response. This exploratory study seeks to improve understanding of metabolic mechanisms in TSC and identify potential targets for precision therapeutic strategies.
Call published on 7 April 2026.
