Marini Carla, Hardies Katia, Pisano Tiziana, May Patrick, Weckhuysen Sarah, Cellini Elena, Suls Arvid, Mei Davide, Balling Rudi, Jonghe Peter D, Helbig Ingo, Garozzo Domenico, Guerrini Renzo
Neurology Unit and Neurogenetics Laboratories, Meyer Children Hospital, Florence, Italy.
Neurogenetics Group, VIB-Department of Molecular Genetics, University of Antwerp, Antwerp, Belgium.
Am J Med Genet A. 2017 Apr;173(4):1119-1123. doi: 10.1002/ajmg.a.38112.
We describe the clinical and whole genome sequencing (WGS) study of a non-consanguineous Italian family in which two siblings, a boy and a girl, manifesting a severe epileptic encephalopathy (EE) with skeletal abnormalities, carried novel SLC35A3 compound heterozygous mutations. Both siblings exhibited infantile spasms, associated with focal, and tonic vibratory seizures from early infancy. EEG recordings showed a suppression-burst (SB) pattern and multifocal paroxysmal activity in both. In addition both had quadriplegia, acquired microcephaly, and severe intellectual disability. General examination showed distal arthrogryposis predominant in the hands in both siblings and severe left dorso-lumbar convex scoliosis in one. WGS of the siblings-parents quartet identified novel compound heterozygous mutations in SLC35A3 in both children. SLC35A3 encodes the major Golgi uridine diphosphate N-acetylglucosamine transporter. With this study, we add SLC35A3 to the gene list of epilepsies. Neurological symptoms and skeletal abnormalities might result from impaired glycosylation of proteins involved in normal development and function of the central nervous system and skeletal apparatus.
我们描述了一个非近亲结婚的意大利家庭的临床及全基因组测序(WGS)研究。该家庭中,一名男孩和一名女孩这两名兄弟姐妹表现出伴有骨骼异常的严重癫痫性脑病(EE),并携带新的SLC35A3复合杂合突变。两名兄弟姐妹均表现出婴儿痉挛症,从婴儿早期就伴有局灶性和强直性振动性发作。脑电图记录显示两人均有抑制-爆发(SB)模式和多灶性阵发性活动。此外,两人均有四肢瘫痪、后天性小头畸形和严重智力残疾。全身检查显示,两名兄弟姐妹双手均以远端关节挛缩为主,其中一人有严重的左背腰段脊柱侧凸。对这对兄弟姐妹及其父母四人进行的全基因组测序在两名儿童中均发现了SLC35A3中的新复合杂合突变。SLC35A3编码主要的高尔基体尿苷二磷酸N-乙酰葡糖胺转运蛋白。通过这项研究,我们将SLC35A3添加到癫痫相关基因列表中。神经症状和骨骼异常可能是由于参与中枢神经系统和骨骼装置正常发育及功能的蛋白质糖基化受损所致。
