van der Knaap Marjo S, Pronk Jan C, Scheper Gert C
Department of Pediatrics and Child Neurology, VU University Medical Center, Amsterdam, Netherlands.
Lancet Neurol. 2006 May;5(5):413-23. doi: 10.1016/S1474-4422(06)70440-9.
Vanishing white matter disease (VWM) is one of the most prevalent inherited childhood leucoencephalopathies. The classical phenotype is characterised by early childhood onset of chronic neurological deterioration, dominated by cerebellar ataxia. VWM is unusual because of its clinically evident sensitivity to febrile infections, minor head trauma, and acute fright, which may cause rapid neurological deterioration and unexplained coma. Most patients die a few years after onset. The phenotypic variation is extremely wide, including antenatal onset and early demise and adult-onset, slowly progressive disease. MRI findings are diagnostic in almost all patients and are indicative of vanishing of the cerebral white matter. The basic defect of this striking disease resides in either one of the five subunits of eukaryotic translation initiation factor eIF2B. eIF2B is essential in all cells of the body for protein synthesis and its regulation under different stress conditions. Although the defect is in housekeeping genes, oligodendrocytes and astrocytes are predominantly affected, whereas other cell types are surprisingly spared. Recently, undue activation of the unfolded-protein response has emerged as important in the pathophysiology of VWM, but the selective vulnerability of glia for defects in eIF2B is poorly understood.
消失性白质病(VWM)是最常见的遗传性儿童白质脑病之一。其经典表型的特征是在儿童早期出现慢性神经功能恶化,以小脑共济失调为主。VWM不同寻常之处在于其对发热感染、轻微头部外伤和急性惊吓具有明显的临床敏感性,这些情况可能导致迅速的神经功能恶化和不明原因的昏迷。大多数患者在发病后几年内死亡。其表型变异范围极广,包括产前发病和早期死亡以及成人发病的缓慢进展性疾病。几乎所有患者的MRI表现都具有诊断意义,提示脑白质消失。这种显著疾病的基本缺陷存在于真核翻译起始因子eIF2B的五个亚基中的任何一个。eIF2B在身体所有细胞中对于蛋白质合成及其在不同应激条件下的调节至关重要。尽管缺陷存在于管家基因中,但少突胶质细胞和星形胶质细胞受到的影响最为显著,而其他细胞类型却出人意料地未受影响。最近,未折叠蛋白反应的过度激活在VWM的病理生理学中已被证明很重要,但对于eIF2B缺陷导致胶质细胞选择性易损性的原因却知之甚少。
