Our patient was a 3-year-old boy with no medical history of interest except for non-isoimmune neonatal jaundice, which required no phototherapy. He displayed normal psychomotor development. According to his parents, 3 weeks before symptom onset, our patient had displayed behavioural changes (irritability with no apparent cause) and slept more hours than usual. One week before symptom onset he showed symptoms of viral infection and common cold and experienced nausea but was afebrile.

He was brought to hospital due to an episode of right-sided deviation of head and eyes and head nodding lasting a few seconds. On the same day, he experienced a similar episode while awake and another while asleep. During this last episode, he sat up with his upper limbs in flexion and displayed right-sided deviation of head and eyes and head clonus, which resolved spontaneously after a few seconds. After this episode, our patient fell onto his back and was drowsy. The frequency of these episodes increased in the following days.

We started treatment with valproic acid and subsequently added intravenous levetiracetam and phenytoin. However, seizures increased and became continuous. At this point, our patient received midazolam infusion and was put into a barbiturate-induced coma for seizure control. In addition to these measures, our patient began a ketogenic diet. He also received intravenous lacosamide, which led to a decrease in the number of seizures. The video-EEG trace, however, revealed epileptiform activity which was nearly continuous in the frontal region of the left hemisphere and maximal in the frontopolar region; signs of focal motor status epilepticus were seen in the oro-lingual-facial region and the right hand. These findings were compatible with EPC (Fig. 1). We conducted several complementary tests to determine the cause of EPC (serology test, tests for neurotropic viruses and oligoclonal bands in CSF, test for serum and CSF NMDA-receptor antibodies, metabolic study, karyotyping, and MRI on 2 occasions); test results were all normal. A subsequent 3-T MRI scan revealed findings suggestive of focal dysplasia at the bottom of the left superior frontal sulcus; the PET scan displayed hypermetabolism in that area (Fig. 2).

Figure 1.

Video-EEG. Continuous epileptiform activity on the left frontal region in the form of 5-Hz rhythmic spikes (EEG activity recorded during barbiturate-induced coma).

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Figure 2.

High-resolution (3-T) T1-weighted MRI scan (coronal section) revealing dysplasia at the bottom of the left superior frontal sulcus (loss of differentiation between grey and white matter).

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Given that our patient had drug-resistant epilepsy, we opted for emergency surgery. We performed left frontal lobectomy to remove the area displaying CD. The anatomical pathology study confirmed the presence of type IIa focal CD.

A follow-up MRI scan performed 6 months after surgery revealed no remnants of dysplastic tissue. The patient was seizure-free. At our most recent follow-up consultation, he was receiving a single antiepileptic agent.