The ILAE now consider that there is insufficient evidence for mechanistic differences between LKS and CSWS to warrant considering them separate syndromes, and proposed the term of “epileptic encephalopathy with CSWS including LKS” for this particular childhood epileptic syndrome (Engel 2006).

Definition of epileptic encephalopathy with CSWS

There is now a large consensus to consider epileptic encephalopathy with CSWS as a spectrum of epileptic conditions defined by (1) an onset in childhood (3y to 10y); (2) the occurrence of cognitive or behavioral impairments that appear or worsen after the epilepsy onset; and (3) the presence of abundant IEDs during sleep, which tend to be more frequent, with increased amplitude and diffusion over the whole scalp during non-rapid eye movement sleep than during the awake state. LKS is a particular presentation in which acquired aphasia is the core symptom. Seizures are not a mandatory feature. When they occur, seizures have variable semiology (focal seizures without consciousness impairment, secondary generalized tonic–clonic seizures, focal negative myoclonia, atypical absences) but, unlike in Lennox–Gastaut syndrome, tonic seizures are usually not encountered (Galanopoulou et al. 2000; Tassinari et al. 2000).

Also, the minimal cognitive impairment needed to make a diagnosis of epileptic encephalopathy with CSWS is a subject of controversy. Indeed, numerous studies have reported an unexpected high rate of cognitive difficulties in the language, attentional, and memory domains in children with classic BECTS, which were associated with IED severity at the acute phase of the disease and resolved with the normalization of the EEG (Deonna 2000; Baglietto et al. 2001; Verrotti et al. 2014).

In conclusion, it is widely accepted that BECTS and epileptic encephalopathy with CSWS are the edges of a spectrum in which the most frequent and diffused IEDs during sleep seem to result in the more severe behavioral and cognitive deficits (Stephani and Carlsson 2006; Kramer et al. 2009; Moeller et al. 2013). The nosological limits between these two conditions are thus somewhat arbitrary.

Aetiology

Epileptic encephalopathy with CSWS is one of the childhood focal epileptic syndromes. According to the terminology revised in 2010 (Berg et al. 2010), the underlying aetiology allows classifying patients within one of the following three subgroups: structural/metabolic, genetic, and unknown. The subgroup of unknown aetiology is the most important, representing more than half of the patients. Patients with structural brain lesions identified on magnetic resonance imaging (MRI) are in the structural/metabolic subgroup and represent approximately 20% of the cases. Lesions are usually antenatal cortical malformations (polymicrogyria) or ante/perinatal cortical destructive lesions, but may also be purely subcortical, the association between thalamic perinatal injury and CSWS being well recognized (Guerrini et al. 1998; Guzzetta et al. 2005). These cases have usually preexisting signs of cerebral palsy. Within this subgroup are also patients with preexisting motor and cognitive deficiencies related to chromosomal anomalies (15q deletion for instance) or genetic syndromes such as Rett syndrome (Van Bogaert et al. 2006). In the genetic subgroup are patients with a demonstrated genetic mutation, but those with mutations associated with structural brain lesions (tubulin genes for instances) and those with chromosomal deletions and preexisting psychomotor delay do not belong to this subgroup. Up to now, there is only one gene demonstrated as pathogenic in the genetic subgroup. This gene is called GRIN2A. Mutations of GRIN2A have been identified by three independent research groups (Carvill et al. 2013, Lesca et al. 2013, and Lemke et al. 2013). Patients with GRIN2A mutations represented about 10% to 20% of cohorts of patients with epileptic encephalopathy with CSWS and normal MRI. Phenotypes are LKS or atypical BECTS, but some patients have a typical BECTS phenotype, further underlying the overlap between these two epileptic syndromes. GRIN2A encodes the N-methyl-D-aspartate (NMDA) glutamate receptor a2 subunit, GluN2A. Patients have either inherited or de novo mutations, which affect NMDA receptor function.

Pathophysiology of cognitive regression

It should be noted that complete normalization of the sleep EEG is not always mandatory to obtain clinical improvement. Indeed, besides the percentage of spike–wave complexes during non-rapid eye movement sleep, the diffusion of the epileptic activity over the whole scalp is also important to consider, as children with diffuse CSWS may show spectacular clinical improvement under treatment even if a focus of spikes persists during a high percentage of sleep time (Aeby et al. 2005; Buzatu et al. 2009).