SHQ1-associated neurodevelopmental disorder: Report of the first homozygous variant in unrelated patients and review of the literature.

IF 1 Q4 GENETICS & HEREDITY

Human Genome Variation Pub Date : 2023-02-22 DOI:10.1038/s41439-023-00234-z

Aljouhra AlHargan, Mohammed A AlMuhaizea, Rawan Almass, Ali H Alwadei, Maha Daghestani, Stefan T Arold, Namik Kaya

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Abstract

Compound heterozygous mutations in SHQ1 have been associated with a rare and severe neurological disorder characterized by global developmental delay (GDD), cerebellar degeneration coupled with seizures, and early-onset dystonia. Currently, only five affected individuals have been documented in the literature. Here, we report three children from two unrelated families harboring a homozygous variant in the gene but with a milder phenotype than previously described. The patients had GDD and seizures. Magnetic resonance imaging analyses revealed diffuse white matter hypomyelination. Sanger sequencing confirmed the whole-exome sequencing results and revealed full segregation of the missense variant (SHQ1:c.833 T > C; p.I278T) in both families. We performed a comprehensive in silico analysis using different prediction classifiers and structural modeling of the variant. Our findings demonstrate that this novel homozygous variant in SHQ1 is likely to be pathogenic and leads to the clinical features observed in our patients.

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SHQ1相关神经发育障碍：报告首例非亲属关系患者的同基因变异并回顾文献。

SHQ1 的复合杂合突变与一种罕见的严重神经系统疾病有关，这种疾病的特征是全身发育迟缓（GDD）、小脑变性并伴有癫痫发作和早发性肌张力障碍。目前，文献中仅记录了五例受影响的个体。在此，我们报告了来自两个无血缘关系家庭的三名儿童，他们都携带该基因的同源变异体，但其表型比以前描述的要轻。这些患者都有 GDD 和癫痫发作。磁共振成像分析显示他们的白质弥漫性髓鞘减少。桑格测序证实了全外显子组测序的结果，并揭示了该错义变体（SHQ1:c.833 T > C; p.I278T）在两个家族中的完全分离。我们使用不同的预测分类器和结构模型对该变异进行了全面的硅学分析。我们的研究结果表明，SHQ1 中的这一新型同源变体很可能是致病的，并导致我们的患者出现临床特征。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Human Genome Variation Biochemistry, Genetics and Molecular Biology-Genetics

CiteScore

2.30

自引率

0.00%

发文量

审稿时长

13 weeks