一例具有新型ISCA2变体的多线粒体功能障碍综合征4,模拟感染后脑炎。

Child neurology open Pub Date : 2023-10-30 eCollection Date: 2023-01-01 DOI:10.1177/2329048X231210421
Hyungjin Chin, Jaeso Cho, Woo Joong Kim, Soo Yeon Kim, Byung Chan Lim, Ki Joong Kim, Jong Hee Chae
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引用次数: 0

摘要

ISCA2功能丧失导致白细胞营养不良和发育倒退(多线粒体功能障碍综合征4(MMDS4))。我们报告了第一例韩国MMDS4病例,该病例在发热发作后表现为快速发育消退和白质营养不良,类似于感染后脑炎。患者在12个月大之前一直表现出正常发育。13个月大时,在经历了疫苗接种后的发烧一个月后,她很快就发展到无法在无人帮助的情况下坐着,也无法说话。脑脊液分析显示淋巴显性白细胞增多症。血清和CSF的氨基酸分析均显示CSF中甘氨酸含量升高。脑磁共振图像显示弥漫性脑白质营养不良。全外显子组测序显示c.166T>G,p.C56G和c.422A>c,p.Q141P的复合杂合ISCA2变体。除双侧视神经萎缩外,没有发现线粒体疾病的证据。在伴有白细胞营养不良的早发性快速发育消退的病例中,应考虑MMDS4。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

A Case of Multiple Mitochondrial Dysfunctions Syndrome 4 with Novel <i>ISCA2</i> Variants, Mimicking Post-Infectious Encephalitis.

A Case of Multiple Mitochondrial Dysfunctions Syndrome 4 with Novel <i>ISCA2</i> Variants, Mimicking Post-Infectious Encephalitis.

A Case of Multiple Mitochondrial Dysfunctions Syndrome 4 with Novel ISCA2 Variants, Mimicking Post-Infectious Encephalitis.

ISCA2 loss of function leads to leukodystrophy and developmental regression (multiple mitochondrial dysfunctions syndrome 4 (MMDS4)). We present a first Korean case of MMDS4 presenting with rapid developmental regression and leukodystrophy after febrile episode, mimicking post-infectious encephalitis. The patient had displayed normal development until 12 months of age. At 13 months of age, one month after experiencing a post-vaccination fever, she quickly progressed to being unable to sit unassisted nor speak any words. Analysis of the cerebrospinal fluid (CSF) revealed lympho-dominant pleocytosis. Amino acid analysis of both the serum and CSF demonstrated elevated glycine exclusively in the CSF. Diffuse leukodystrophy was noted in the brain magnetic resonance image. Whole exome sequencing revealed compound heterozygous ISCA2 variants of c.166T>G, p.C56G and c.422A>C, p.Q141P. No evidence of mitochondrial disease other than bilateral optic atrophy was noted. In cases of early onset rapid developmental regression with leukodystrophy, MMDS4 should be considered.

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