先天性肌无力综合征2个兄弟姐妹CHRNE基因的新纯合变异。

Child neurology open Pub Date : 2023-11-28 eCollection Date: 2023-01-01 DOI:10.1177/2329048X231216432
Cassie Chan, Lucy Emery, Caroline Maltese, Ashutosh Kumar, Ermal Aliu, Sunil Naik, Dustin Paul
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引用次数: 0

摘要

胆碱能受体烟碱epsilon (CHRNE)亚基突变引起突触后型先天性肌无力综合征,可能是原发性乙酰胆碱受体缺乏或受体通道动力学异常。我们报告了一种新的纯合变异(c.322C > T, p.Pro108Ser)在epsilon亚基中引起两个兄弟姐妹的原发性乙酰胆碱受体缺乏。两个兄弟姐妹表现出疲惫的虚弱。两个兄弟姐妹的全外显子组测序显示,在epsilon亚基上存在未知意义的纯合子变异(c.322C > T, p.Pro108Ser)。肌电图/神经传导研究与重复神经刺激的一个兄弟姐妹显示神经肌肉连接传递缺陷。伪麻黄碱和氟西汀对疑似慢通道先天性肌无力综合征无改善作用。吡哆斯的明试验导致临床改善。结合临床表现、亲缘关系、纯合遗传变异和对吡斯的明的反应,我们认为是胆碱能受体烟碱epsilon亚基纯合变异(c.322C > T, p.Pro108Ser)导致原发性乙酰胆碱受体缺乏性先天性肌无力综合征。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
A Novel Homozygous Variant in the CHRNE Gene in 2 Siblings with Congenital Myasthenic Syndrome.

Cholinergic receptor nicotinic epsilon (CHRNE) subunit mutations cause postsynaptic type of congenital myasthenic syndrome either as a primary acetylcholine-receptor deficiency or abnormal channel kinetics in the receptor. We report a novel homozygous variant (c.322C > T, p.Pro108Ser) in the epsilon subunit causing primary acetylcholine-receptor deficiency in two siblings. Two siblings presented with fatigable weakness. Both siblings had whole exome sequencing showing a homozygous variant (c.322C > T, p.Pro108Ser) of unknown significance in the epsilon subunit. Electromyography/nerve conduction study with repetitive nerve stimulation on one sibling showed a defect in neuromuscular junction transmission. Pseudoephedrine and fluoxetine for suspected slow-channel congenital myasthenic syndrome yielded no improvement. A trial of pyridostigmine led to clinical improvement. Given the clinical presentation, consanguinity, homozygous genetic variant, and response to pyridostigmine, we rationalize the homozygous variant (c.322C > T, p.Pro108Ser) in cholinergic receptor nicotinic epsilon subunit causes the primary acetylcholine-receptor deficiency congenital myasthenic syndrome.

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