Cossu Alberto, Santos Joana L, Galati Giulia, Nikanorova Marina, Costa Paola, Mang Yuan, Silahtaroglu Asli, Rubboli Guido, Tommerup Niels, Dalla Bernardina Bernardo, Møller Rikke S, Cantalupo Gaetano, Gardella Elena
Danish Epilepsy Centre, Dianalund, Denmark.
Centro di Ricerca per Epilessia in età Pediatrica (CREP), AOUI, Verona, Italy.
Neurol Sci. 2023 Jun;44(6):2173-2176. doi: 10.1007/s10072-023-06735-7. Epub 2023 Mar 13.
Heterozygous variants in PRRT2 are mostly associated with benign phenotypes, being the major genetic cause of benign familial infantile seizures (BFIS), as well as in paroxysmal disorders. We report two children from unrelated families with BFIS that evolved to encephalopathy related to status epilepticus during sleep (ESES).
Two probands presented with focal motor seizures at 3 months of age, with a limited course. Both children presented, at around 5 years of age, with centro-temporal interictal epileptiform discharges with a source in the frontal operculum, markedly activated by sleep, and associated with stagnation on neuropsychological development. Whole-exome sequencing and co-segregation analysis revealed a frameshift mutation c.649dupC in the proline-rich transmembrane protein 2 (PRRT2) in both probands and all affected family members.
The mechanism leading to epilepsy and the phenotypic variability of PRRT2 variants remain poorly understood. However, its wide cortical and subcortical expression, in particular in the thalamus, could partially explain both the focal EEG pattern and the evolution to ESES. No variants in the PRRT2 gene have been previously reported in patients with ESES. Due to the rarity of this phenotype, other possible causative cofactors are likely contributing to the more severe course of BFIS in our probands.
富含脯氨酸的跨膜蛋白2(PRRT2)中的杂合变异大多与良性表型相关,是良性家族性婴儿惊厥(BFIS)以及阵发性疾病的主要遗传原因。我们报告了来自两个无亲缘关系家庭的患有BFIS的儿童,其病情在睡眠期间演变为与癫痫持续状态(ESES)相关的脑病。
两名先证者在3个月大时出现局灶性运动性惊厥,病程有限。两个孩子在大约5岁时均出现中央颞区发作间期癫痫样放电,起源于额盖,睡眠时明显激活,并伴有神经心理发育停滞。全外显子组测序和共分离分析显示,两名先证者及其所有受影响的家庭成员中,富含脯氨酸的跨膜蛋白2(PRRT2)存在移码突变c.649dupC。
导致癫痫的机制以及PRRT2变异的表型变异性仍知之甚少。然而,其在广泛的皮质和皮质下表达,尤其是在丘脑中的表达,可能部分解释了脑电图的局灶性模式以及向ESES的演变。此前尚无ESES患者PRRT2基因变异的报道。由于这种表型罕见,其他可能的致病辅助因素可能导致了我们先证者中BFIS病程更为严重。
