Dravet syndrome as part of the clinical and genetic spectrum of sodium channel epilepsies and encephalopathies

Mei, Davide; Cetica, Valentina; Marini, Carla; Guerrini, Renzo

doi:10.1111/epi.16054

Cited by 51 publications

(63 citation statements)

References 57 publications

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“…It is possible -and perhaps likely -that mice remaining alive represent a nonrandom subset of the initial population. It is well known that there is a spectrum of disease severity in Scn1a+/mice , similar to that observed in humans [Harkin et al, 2007, Mei et al, 2019, the basis of which is unclear but may involve genetic modifiers , Calhoun et al, 2017. This concern may pertain to any study involving an experimental animal model of a neurodevelopmental disorder associated with mortality.…”

Section: Introductionmentioning

confidence: 85%

Developmentally-regulated impairment of parvalbumin interneuron synaptic transmission in an experimental model of Dravet syndrome

Kaneko

Currin

Goff

et al. 2021

Preprint

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Dravet syndrome (DS) is a neurodevelopmental disorder defined by epilepsy, intellectual disability, and sudden death, due to heterozygous variants in SCN1A with loss of function of the sodium channel subunit Nav1.1. Nav1.1-expressing parvalbumin GABAergic interneurons (PV-INs) from pre-weanling Scn1a+/- mice show impaired action potential generation. A novel approach assessing PV-IN function in the same mice at two developmental time points showed that, at post-natal day (P) 16-21, spike generation was impaired all mice, deceased prior or surviving to P35. However, synaptic transmission was selectively dysfunctional in pre-weanling mice that did not survive. Spike generation in surviving mice normalized by P35, yet we again identified abnormalities in synaptic transmission. We conclude that combined dysfunction of PV-IN spike generation and synaptic transmission drives disease severity, while ongoing dysfunction of synaptic transmission contributes to chronic pathology. Modeling revealed that PV-IN axonal propagation is more sensitive to decreases in sodium conductance than spike generation.

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Section: Introductionmentioning

confidence: 85%

Developmentally-regulated impairment of parvalbumin interneuron synaptic transmission in an experimental model of Dravet syndrome

Kaneko

Currin

Goff

et al. 2021

Preprint

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“…Over 150 mutations in the SCN1A gene have been described. Another form of epilepsy connected with SCN1A mutations, apart from DS, is epilepsy with febrile seizures plus and epilepsy of infancy with migrating focal seizures [ 1 , 2 , 3 , 4 ]. Familial hemiplegic migraine also may be caused by abnormalities within SCN1A gene [ 1 , 2 , 3 , 4 ].…”

Section: Discussionmentioning

confidence: 99%

“…About 75–85% of individuals affected by DS have loss-of-function mutations in the SCN1A gene encoding the sodium channel alpha subunit [ 2 ]. In SCN1A mutation negative patients with clinical similarity to DS, different genetic background is found, particularly the following gene mutations: PCDH19 , CHD2 , STXBP1 , HCN1 , GABRG2 , GABRA1 , and SCN1B [ 3 ].…”

Section: Introductionmentioning

confidence: 99%

Dravet Syndrome—The Polish Family’s Perspective Study

Paprocka

Lewandowska

Zieliński

et al. 2021

JCM

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Aim: The aim of the paper is to study the prevalence of Dravet Syndrome (DS) in the Polish population and indicate different factors other than seizures reducing the quality of life in such patients. Method: A survey was conducted among caregivers of patients with DS by the members of the Polish support group of the Association for People with Severe Refractory Epilepsy DRAVET.PL. It included their experience of the diagnosis, seizures, and treatment-related adverse effects. The caregivers also completed the PedsQL survey, which showed the most important problems. The survey received 55 responses from caregivers of patients with DS (aged 2–25 years). Results: Prior to the diagnosis of DS, 85% of patients presented with status epilepticus lasting more than 30 min, and the frequency of seizures (mostly tonic-clonic or hemiconvulsions) ranged from 2 per week to hundreds per day. After the diagnosis of DS, patients remained on polytherapy (drugs recommended in DS). Before diagnosis, some of them had been on sodium channel blockers. Most patients experienced many adverse effects, including aggression and loss of appetite. The frequency of adverse effects was related to the number of drugs used in this therapy, which had an impact on the results of the PedsQL form, particularly in terms of the physical and social spheres. Intensive care unit stays due to severe status epilepticus also had an influence on the results of the PedsQL form. Conclusions: Families must be counseled on non-pharmacologic strategies to reduce seizure risk, including avoidance of triggers that commonly induce seizures (including hyperthermia, flashing lights and patterns, sleep abnormalities). In addition to addressing seizures, holistic care for a patient with Dravet syndrome must involve a multidisciplinary team that includes specialists in physical, occupational and speech therapy, neuropsychology, social work.

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“…Precision medicine: novel treatment strategies developed from pathophysiological knowledge 3. Precision medicine: aetiology-based preventive treatments and in progress treatments Clinical-based evidence of known ASM modifying -either worsening or improving -seizure frequency One of the first and best example of how the identification of the underling genetic aetiology guides treatment is that of Dravet Syndrome (DS) the most renowned and studied developmental and epileptic encephalopathy (DEE) (Mei et al 2019). Well before the genetic cause was identified, some clinical reports indicated that sodium channel blockers including lamotrigine (LTG) and carbamazepine (CBZ) should be avoided in patients with DS since they have the potential to determine an increase in seizure frequency evolving to status epilepticus in some patients (Guerrini et al, 1998;de Lange et al 2018).…”

Section: Introductionmentioning

confidence: 99%

“…Well before the genetic cause was identified, some clinical reports indicated that sodium channel blockers including lamotrigine (LTG) and carbamazepine (CBZ) should be avoided in patients with DS since they have the potential to determine an increase in seizure frequency evolving to status epilepticus in some patients (Guerrini et al, 1998;de Lange et al 2018). Following the discovery that DS is associated to mutations of the alpha1 subunit of the sodium channel (SCN1A) possibly causing loss of channel function, the clinical evidence that the administration of sodium channel blockers made seizure worse was partly explained (Claes et al 2001;Mantegazza, Marini 2010;Mei et al 2019). Although complete seizure control is rarely attainable, clinical studies have shown that the combination of valproic acid (VPA), clobazam (CLB) and stiripentol (STP) is the most effective in preventing seizures especially avoiding the evolution into status epilepticus, frequently observed in infants with DS (Ceulemans et al 2004;Wirrel et al 2018, Wirrel andNabbout 2019).…”

Section: Introductionmentioning

confidence: 99%

Novel treatments in Epilepsy guided by Genetic Diagnosis

Marini

Giardino

2021

Preprint

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Identifying the optimal treatment based on specific aetiology of each patient is the main promise of precision medicine. In order to realize this promise researches and physicians must first identify the underlying cause; over the last 10 years, advances in genetics have made this possible for several monogenic epilepsies. At present through next generation techniques we can reach the precise genetic aetiology in 30 to 50% of genetic epilepsies beginning in the paediatric age. While committed in such gene hunting, progresses in the study of experimental models of epilepsy have also provided a better understanding of the mechanisms underlying the condition. Such impressive advances is already being translated into improving care, management and treatment of some patients. Identification of a precise genetic etiology can already direct physicians to prescribe treatments correcting specific metabolic defects avoid antiseizure medicines that can aggravate the pathogenic defect or select the drug that counteract the functional disturbance caused by the gene mutation. Personalized, tailored treatments should not just focus on how to stop seizures but possibly preventing their onset and cure the disorder often consisting of epilepsy and its comorbidities including cognitive, motor and behavior deficiencies. This review discusses the therapeutic implications following a specific genetic diagnosis and the correlation between genetic findings, pathophysiological mechanism and tailored seizure treatment emphasizing the impact on current clinical practice.

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Dravet syndrome as part of the clinical and genetic spectrum of sodium channel epilepsies and encephalopathies

Cited by 51 publications

References 57 publications

Developmentally-regulated impairment of parvalbumin interneuron synaptic transmission in an experimental model of Dravet syndrome

Developmentally-regulated impairment of parvalbumin interneuron synaptic transmission in an experimental model of Dravet syndrome

Dravet Syndrome—The Polish Family’s Perspective Study

Novel treatments in Epilepsy guided by Genetic Diagnosis

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