Cohen syndrome: Can early-onset recurrent infections and hypotonia provide early diagnosis and intervention for intellectual disability?

IF 1.7 4区医学 Q3 DEVELOPMENTAL BIOLOGY International Journal of Developmental Neuroscience Pub Date : 2024-10-13 DOI:10.1002/jdn.10384

Gül Ünsel-Bolat, Ezgi Keskin-Çelebi, Hilmi Bolat

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Abstract

Introduction

Cohen syndrome is a rare disease associated with neurodevelopmental disorders, especially intellectual disability (ID), neutropenia and recurrent infections are consistently reported in cases. Neutropenia is an important part of the syndrome, as well as ID. Homozygous variants in the VPS13B gene, located on chromosome 8q22 and containing 62 exons, have been found to cause Cohen syndrome. Cohen syndrome is commonly diagnosed when dysmorphological findings and developmental delay become more apparent. However, the identification of some findings with increasing age has caused the diagnosis of Cohen syndrome to be delayed.

Methods

Cases diagnosed with ID were evaluated using whole-exome sequencing/clinical exome sequencing method. Family segregation analysis was performed using Sanger sequencing. We presented the clinical and genetic findings of three cases diagnosed with Cohen syndrome and their parents in detail.

Results

In this study, we presented the occurrence of symptoms in different age groups, and the prognosis of three cases carrying the VPS13B gene variants, including three different variant types: missense, frameshift and nonsense. Although our cases had different variant types, they shared important similarities on the onset period and prognosis of the symptoms. All cases presented hypotonia, difficulties in swallowing, recurrent respiratory tract infections, neutropenia, delay in motor development, ID and hyperactivity. Our cases did not have a diagnosis of autism spectrum disorder. All cases had increased willingness to engage in social communication.

Conclusion

We emphasize the importance of early-onset recurrent infections and hypotonia for early diagnosis and preventive genetic counselling in Cohen syndrome.

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科恩综合征：早期反复感染和肌张力低下能否为智力障碍提供早期诊断和干预？

导言科恩综合征是一种罕见的疾病，伴有神经发育障碍，尤其是智力障碍（ID）、中性粒细胞减少症和反复感染。中性粒细胞减少症是该综合征的重要组成部分，同时也是智力障碍。VPS13B 基因位于染色体 8q22，包含 62 个外显子，已发现该基因的同源变异可导致科恩综合征。科恩综合征通常在畸形和发育迟缓变得更加明显时才被诊断出来。然而，随着年龄的增长，一些结果的确定导致科恩综合征的诊断被推迟：方法：采用全外显子组测序/临床外显子组测序方法对确诊为ID的病例进行评估。采用桑格测序法进行家族分离分析。我们详细介绍了确诊为科恩综合征的三个病例及其父母的临床和遗传学结果：在这项研究中，我们介绍了三个携带 VPS13B 基因变异的病例在不同年龄段的症状发生情况和预后，其中包括三种不同的变异类型：错义、框移和无义。虽然我们的病例有不同的变异类型，但它们在发病期和预后方面有重要的相似之处。所有病例均表现为肌张力低下、吞咽困难、反复呼吸道感染、中性粒细胞减少、运动发育迟缓、智障和多动。我们的病例没有自闭症谱系障碍的诊断。所有病例都更愿意参与社会交流：我们强调，早期出现的反复感染和肌张力低下对科恩综合征的早期诊断和预防性遗传咨询非常重要。

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

International Journal of Developmental Neuroscience 医学-发育生物学

CiteScore

3.30

自引率

5.60%

发文量

审稿时长

6-12 weeks

期刊介绍： International Journal of Developmental Neuroscience publishes original research articles and critical review papers on all fundamental and clinical aspects of nervous system development, renewal and regeneration, as well as on the effects of genetic and environmental perturbations of brain development and homeostasis leading to neurodevelopmental disorders and neurological conditions. Studies describing the involvement of stem cells in nervous system maintenance and disease (including brain tumours), stem cell-based approaches for the investigation of neurodegenerative diseases, roles of neuroinflammation in development and disease, and neuroevolution are also encouraged. Investigations using molecular, cellular, physiological, genetic and epigenetic approaches in model systems ranging from simple invertebrates to human iPSC-based 2D and 3D models are encouraged, as are studies using experimental models that provide behavioural or evolutionary insights. The journal also publishes Special Issues dealing with topics at the cutting edge of research edited by Guest Editors appointed by the Editor in Chief. A major aim of the journal is to facilitate the transfer of fundamental studies of nervous system development, maintenance, and disease to clinical applications. The journal thus intends to disseminate valuable information for both biologists and physicians. International Journal of Developmental Neuroscience is owned and supported by The International Society for Developmental Neuroscience (ISDN), an organization of scientists interested in advancing developmental neuroscience research in the broadest sense.