Cho Kye Hee, Shim Sung Han, Jung Youngsoo, Sung Se Ra, Kim MinYoung
Department of Rehabilitation Medicine, CHA Bundang Medical Center, CHA University, 59 Yatap-ro, Bundang-gu, Seongnam, Gyeonggi-do, 13496, Republic of Korea.
Department of Biomedical Science, College of Life Science, CHA University, 120 Haeryong-ro, Pochun, Gyeonggi-do, 11160, Republic of Korea.
BMC Med Genet. 2018 Aug 29;19(1):152. doi: 10.1186/s12881-018-0663-0.
Sjogren-Larsson syndrome is a hereditary neurocutaneous syndrome that is non-progressive in nature. Although neuroregression has been reported in seizure-prone preschool children requiring anti-epileptic treatment, teenage-onset dystonia precipitating neurodegeneration without any immediate causal events has yet to be reported.
We describe a young woman with spastic diplegia and intellectual disability who began to show progressive neurological deterioration from 12 years of age, with the onset of dystonia and tremor. She was initially diagnosed with spastic cerebral palsy and periventricular leukomalacia based on brain magnetic resonance imaging. Follow-up brain imaging from 13 years of age did not reveal apparent changes, though abnormal electroencephalographic findings occurred in parallel with her decline in motor function. By 19 years of age, she had developed dysphagia and became completely dependent on others for most activities of daily living. Ultimately, whole-exome sequencing revealed a heterozygous compound mutation in the ALDH3A2 gene that corresponds to Sjogren-Larsson syndrome: an exon 9 deletion (1291-1292delAA) from the mother and an exon 5 splicing mutation (798 + 1delG) from the father. Neuroregression has been reported in preschool children after seizures requiring treatment, though our patient did not experience any immediate causal events. This report summarizes the clinical, radiologic, and electrophysiological findings observed over a decade concurrent with neurological deterioration after the onset of dystonia and tremor at the age of developmental ceiling in Sjogren-Larsson syndrome.
In addition to the influence of additive variants or other environmental factors, accumulation of metabolites due to defective fatty aldehyde dehydrogenase is a potential pathomechanism of neurodegeneration in this patient. Neurological deterioration may be a presentation that is unnoticed in Sjogren-Larsson syndrome due to the rarity of the disease. This report highlights a unique clinical feature of Sjogren-Larsson syndrome with progressive neurodegeneration associated with dystonia and tremor.
舍格伦-拉尔松综合征是一种遗传性神经皮肤综合征,本质上是非进行性的。虽然已有报道称,易癫痫发作的学龄前儿童在接受抗癫痫治疗后会出现神经功能退化,但青少年期起病的肌张力障碍导致神经退行性变且无任何直接病因事件的情况尚未见报道。
我们描述了一名患有痉挛性双瘫和智力残疾的年轻女性,她从12岁开始出现进行性神经功能恶化,伴有肌张力障碍和震颤。根据脑部磁共振成像,她最初被诊断为痉挛性脑瘫和脑室周围白质软化症。13岁时的后续脑部成像未发现明显变化,不过异常脑电图结果与她运动功能的下降同时出现。到19岁时,她出现了吞咽困难,在大多数日常生活活动中完全依赖他人。最终,全外显子组测序显示ALDH3A2基因存在杂合复合突变,符合舍格伦-拉尔松综合征:来自母亲的外显子9缺失(1291 - 1292delAA)和来自父亲的外显子5剪接突变(798 + 1delG)。已有报道称癫痫发作后接受治疗的学龄前儿童会出现神经功能退化,不过我们的患者未经历任何直接病因事件。本报告总结了在舍格伦-拉尔松综合征发育上限年龄出现肌张力障碍和震颤后,伴随神经功能恶化的十年间观察到的临床、放射学和电生理结果。
除了累加变异或其他环境因素的影响外,脂肪醛脱氢酶缺陷导致的代谢产物积累是该患者神经退行性变的潜在发病机制。由于该病罕见,神经功能恶化可能是舍格伦-拉尔松综合征中未被注意到的一种表现。本报告突出了舍格伦-拉尔松综合征伴有与肌张力障碍和震颤相关的进行性神经退行性变的独特临床特征。
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