Klingelhoefer Lisa, Misbahuddin Anjum, Jawad Tania, Mellers John, Jarosz Jozef, Weeks Robert, Ray Chaudhuri Kallol
Department of Neurology, National Parkinson Foundation International Centre of Excellence, King's College Hospital and King's College, London, United Kingdom; Department of Neurology, Technical University Dresden, Dresden, Germany.
Essex Centre for Neurological Sciences, Romford, United Kingdom.
Pediatr Neurol. 2014 Jul;51(1):157-64. doi: 10.1016/j.pediatrneurol.2014.03.008. Epub 2014 Mar 15.
Vanishing white matter disease is caused by mutations of the eukaryotic translation initiation factor 2B (EIF2B) and is a prevalent cause of inherited childhood leukoencephalopathy. Infantile and early childhood onset forms are associated with chronic progressive neurological signs, with episodes of rapid, neurological, and poor prognosis, with death in few months or years. In contrast, onset in late childhood and adult onset is rare and is associated with long-term survival because of milder signs and slow progression.
We present a patient with a genetically proven vanishing white matter disease, typical brain MRI, presenting with opsoclonus myoclonus in early childhood and a delayed development of adult multifocal dystonia and schizoaffective disorder with continued survival. In addition we have also reviewed the relevant literature based on 42 previous articles summarizing clinical details of 318 individuals with vanishing white matter disease (single case reports to case series). In 283, genetic mutation of EIF2B was confirmed with the onset of vanishing white matter disease reported as antenatal (seven), infantile (eight), early childhood (107), between infantile and early childhood (20), late childhood (25), between early and late childhood (three), adult (68), and between late childhood and adult (21).
Various movement disorders have been described with vanishing white matter disease either at presentation (mimicking an opsoclonus myoclonus syndrome) or in adulthood (dystonia and myoclonus) with continuing survival. Relatively preserved cognition is a novel presentation and is reported in this article along with a comprehensive literature review.
消失性白质病由真核生物翻译起始因子2B(EIF2B)突变引起,是遗传性儿童白质脑病的常见病因。婴儿期和幼儿期发病形式与慢性进行性神经体征相关,伴有快速进展的神经功能障碍和预后不良,在数月或数年内死亡。相比之下,儿童晚期和成人期发病较为罕见,由于体征较轻和进展缓慢,患者可长期存活。
我们报告1例经基因证实的消失性白质病患者,其具有典型的脑部MRI表现,在幼儿期出现眼阵挛-肌阵挛,成年后出现迟发性多灶性肌张力障碍和分裂情感性障碍,并持续存活。此外,我们还根据之前的42篇文章回顾了相关文献,总结了318例消失性白质病患者的临床细节(从单病例报告到病例系列)。在283例中,证实存在EIF2B基因突变,消失性白质病的发病情况报告为产前(7例)、婴儿期(8例)、幼儿期(107例)、婴儿期与幼儿期之间(20例)、儿童晚期(25例)、儿童早期与晚期之间(3例)、成人期(68例)以及儿童晚期与成人期之间(21例)。
消失性白质病患者在发病时(类似眼阵挛-肌阵挛综合征)或成年后(肌张力障碍和肌阵挛)会出现各种运动障碍,且患者持续存活。相对保留的认知功能是一种新的表现形式,本文对此进行了报道,并进行了全面的文献综述。
