Extensive, 3.8 Mb-Sized Deletion of 22q12 in a Patient with Bilateral Schwannoma, Intellectual Disability, Sensorineural Hearing Loss, and Epilepsy.

IF 0.9 4区医学 Q4 GENETICS & HEREDITY

Molecular Syndromology Pub Date : 2023-10-01 Epub Date: 2023-06-02 DOI:10.1159/000528744

Jakub Trizuljak, Jakub Duben, Ivona Blaháková, Zuzana Vrzalová, Kateřina Staňo Kozubík, Jiří Štika, Lenka Radová, Veronika Bergerová, Soňa Mejstříková, Věra Hořínová, Radim Jančálek, Šárka Pospíšilová, Michael Doubek

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引用次数: 0

Abstract

Introduction: In contrast with the well-known and described deletion of the 22q11 chromosome region responsible for DiGeorge syndrome, 22q12 deletions are much rarer. Only a few dozen cases have been reported so far. This region contains genes responsible for cell cycle control, chromatin modification, transmembrane signaling, cell adhesion, and neural development, as well as several cancer predisposition genes.

Case presentation: We present a patient with cleft palate, sensorineural hearing loss, vestibular dysfunction, epilepsy, mild to moderate intellectual disability, divergent strabism, pes equinovarus, platyspondylia, and bilateral schwannoma. Using Microarray-based Comparative Genomic Hybridization (aCGH), we identified the de novo 3.8 Mb interstitial deletion at 22q12.1→22q12.3. We confirmed deletion of the critical NF2 region by MLPA analysis.

Discussion: Large 22q12 deletion in the proband encases the critical NF2 region, responsible for development of bilateral schwannoma. We compared the phenotype of the patient with previously reported cases. Interestingly, our patient developed cleft palate even without deletion of the MN1 gene, deemed responsible in previous studies. We also strongly suspect the DEPDC5 gene deletion to be responsible for seizures, consistent with previously reported cases.

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双侧神经鞘瘤、智力残疾、感觉神经性听力损失和癫痫患者22q12的3.8Mb大范围缺失。

引言：与众所周知和描述的导致DiGeorge综合征的22q11染色体区域缺失相比，22q12缺失要罕见得多。到目前为止，只报告了几十例病例。该区域包含负责细胞周期控制、染色质修饰、跨膜信号传导、细胞粘附和神经发育的基因，以及几个癌症易感性基因。病例介绍：我们报告了一名腭裂、感音神经性听力损失、前庭功能障碍、癫痫、轻度至中度智力残疾、发散性斜视、分点内翻足、平板型脊柱炎和双侧神经鞘瘤患者。使用基于微阵列的比较基因组杂交（aCGH），我们在22q12.1处发现了3.8 Mb的间质缺失→22q12.3.我们通过MLPA分析证实了关键NF2区域的缺失。讨论：先证者的22q12大缺失包围了关键的NF2区域，负责双侧神经鞘瘤的发展。我们将患者的表型与先前报道的病例进行了比较。有趣的是，我们的患者在没有MN1基因缺失的情况下也出现了腭裂，这在以前的研究中被认为是罪魁祸首。我们还强烈怀疑DEPDC5基因缺失是癫痫发作的原因，这与之前报道的病例一致。

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来源期刊

Molecular Syndromology Biochemistry, Genetics and Molecular Biology-Genetics

CiteScore

1.70

自引率

9.10%

发文量

期刊介绍： ''Molecular Syndromology'' publishes high-quality research articles, short reports and reviews on common and rare genetic syndromes, aiming to increase clinical understanding through molecular insights. Topics of particular interest are the molecular basis of genetic syndromes, genotype-phenotype correlation, natural history, strategies in disease management and novel therapeutic approaches based on molecular findings. Research on model systems is also welcome, especially when it is obviously relevant to human genetics. With high-quality reviews on current topics the journal aims to facilitate translation of research findings to a clinical setting while also stimulating further research on clinically relevant questions. The journal targets not only medical geneticists and basic biomedical researchers, but also clinicians dealing with genetic syndromes. With four Associate Editors from three continents and a broad international Editorial Board the journal welcomes submissions covering the latest research from around the world.