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2
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3
Vagus nerve stimulation in children with drug-resistant epilepsy of monogenic etiology.迷走神经刺激术治疗单基因病因耐药性癫痫患儿
Front Neurol. 2022 Sep 1;13:951850. doi: 10.3389/fneur.2022.951850. eCollection 2022.
4
Genome sequencing is a sensitive first-line test to diagnose individuals with intellectual disability.基因组测序是诊断智力障碍个体的一种敏感的一线检测方法。
Genet Med. 2022 Nov;24(11):2296-2307. doi: 10.1016/j.gim.2022.07.022. Epub 2022 Sep 6.
5
Whole exome and genome sequencing in mendelian disorders: a diagnostic and health economic analysis.全外显子组和全基因组测序在孟德尔疾病中的应用:一项诊断和健康经济学分析。
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6
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Hum Mutat. 2022 May;43(5):568-581. doi: 10.1002/humu.24347. Epub 2022 Mar 1.
7
Exome first approach to reduce diagnostic costs and time - retrospective analysis of 111 individuals with rare neurodevelopmental disorders.外显子组-first approach 以降低诊断成本和时间-111 例罕见神经发育障碍个体的回顾性分析。
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影响一名小头畸形和眼部异常患者以及一名未出生的脑沟异常同胞的双复合杂合缺失。

Two-Compound Heterozygous Deletions Affecting in a Patient with Microcephaly and Ocular Abnormalities and in an Unborn Sibling with Abnormal Sulcation.

作者信息

Pal Swasti, Kulshrestha Samarth, Garg Neha, Gupta Deepti, Gupta Nandita Dimri, Puri Ratna Dua

机构信息

Institute of Medical Genetics and Genomics Ganga Ram Institute of Post Graduate Medical Education and Research Sir Ganga Ram Hospital, New Delhi, India.

Department of Fetal Medicine, Ganga Ram Institute of Post Graduate Medical Education and Research, Sir Ganga Ram Hospital, New Delhi, India.

出版信息

Mol Syndromol. 2024 Dec;15(6):503-516. doi: 10.1159/000539099. Epub 2024 Jun 10.

DOI:10.1159/000539099
PMID:39634241
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11614437/
Abstract

INTRODUCTION

-related disorder is a known cause of autosomal recessive microcephaly and chorioretinopathy, which was originally recognized as a new syndrome based on unique ocular findings on a phenotypic overlap of microcephalic primordial short stature. Since the elucidation of its molecular mechanism, limited families have been published in literature and the disorder remains rare worldwide.

CASE PRESENTATION

We present the first Indian family with an affected child and sibling fetus with microcephaly, dysmorphism, and agyria/pachygyria complex on brain imaging in both and short stature, intellectual disability, and visual impairment in proband. As for many patients with long diagnostic odysseys, this child also underwent multiple genomic tests. Genome sequencing through the Indian Undiagnosed Disease Program (I-UDP) confirmed the diagnosis in both proband and sibling fetus. Compound heterozygous variants were identified in including an eleven base pair deletion (inherited from father) and 405 base pair large deletion (inherited from mother). Reverse phenotyping to confirm the ocular phenotype in proband confirmed -related microcephaly and chorioretinopathy. We report third trimester microcephaly with ventriculomegaly and abnormal sulcation as part of the antenatal presentation for this condition.

CONCLUSION

This case represents an Indian family with a seemingly obvious clinical diagnosis compounded by a long diagnostic odyssey and the first ever structural variant to be identified via whole genome sequencing in in trans with an indel variant.

摘要

引言

-相关疾病是常染色体隐性小头畸形和脉络膜视网膜病变的已知病因,最初是基于小头原始身材矮小的表型重叠所具有的独特眼部表现而被确认为一种新综合征。自从其分子机制被阐明以来,文献中报道的相关家系有限,该疾病在全球范围内仍然罕见。

病例报告

我们报告了印度的首个家系,家系中的患病儿童及其患病同胞胎儿均患有小头畸形、畸形以及脑成像显示的无脑回/巨脑回复合体,且二者均身材矮小,先证者存在智力障碍和视力损害。和许多诊断历程漫长的患者一样,该患儿也接受了多项基因检测。通过印度未确诊疾病项目(I-UDP)进行的基因组测序在先证者及其患病同胞胎儿中均确诊了该病。在中鉴定出复合杂合变异,包括一个11个碱基对的缺失(从父亲遗传而来)和一个405个碱基对的大片段缺失(从母亲遗传而来)。通过反向表型分析来确认先证者的眼部表型,证实为-相关小头畸形和脉络膜视网膜病变。我们报告了作为该病产前表现一部分的孕晚期小头畸形合并脑室扩大和脑沟异常。

结论

本病例代表了一个印度家系,其临床诊断看似明确,但诊断历程漫长,并且这是通过全基因组测序首次鉴定出的与一个插入缺失变异呈反式构型的结构变异。