双等位基因COL18A1突变引起的后窝畸形伴小脑中线裂畸形的兄弟姐妹Knobloch综合征:基于病例的回顾。

IF 0.4 Q4 PEDIATRICS Journal of pediatric genetics Pub Date : 2023-03-01 DOI:10.1055/s-0040-1721073
Siddaramappa J Patil, Shruti Pande, Jyoti Matalia, Venkatraman Bhat, Minal Kekatpure, Katta Mohan Girisha
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引用次数: 0

摘要

Knobloch综合征(KS)是由COL18A1双等位致病变异引起的常染色体隐性遗传病。KS临床表现为典型的眼部表现(高度近视、玻璃体视网膜变性、视网膜脱离、晶状体半脱位),多变的神经系统表现(枕部脑膨出、多小回畸形、小脑畸形、癫痫、智力残疾),以及其他不常见的临床表现。所有KS患者的文献回顾(来源PubMed)都特别提到了小脑异常。在这里,我们报告两个兄弟姐妹与典型的KS后窝畸形和新型小脑中线裂异常分析全外显子组测序。已知致病性纯合变异体c.2908C > T;COL18A1基因外显子26中的一个基因(p.a g970ter)被发现是导致KS的原因。这两个兄弟姐妹表现为早发性严重眼部表现,面部畸形,中枢神经系统表现变化,并伴有新的小脑中线裂异常。结构性脑畸形和基因型的存在与否并不能绝对预测KS患者的认知功能。然而,后窝异常的存在可能预示着以后生活中共济失调的发展,需要进一步的研究。
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Knobloch Syndrome in Siblings with Posterior Fossa Malformations Along with Cerebellar Midline Cleft Abnormality Caused by Biallelic COL18A1 Mutation: Case-Based Review.

Knobloch syndrome (KS) is an autosomal recessive disorder caused by biallelic pathogenic variants in COL18A1 . KS clinically manifests with the typical eye findings (high myopia, vitreoretinal degeneration, retinal detachment, and lens subluxation), variable neurological findings (occipital encephalocele, polymicrogyria, cerebellar malformations, epilepsy, and intellectual disability), and the other uncommon clinical manifestations. Literature review of all KS patients (source PubMed) was done with special reference to cerebellar abnormalities. Here, we report two siblings with typical KS with posterior fossa malformations and novel cerebellar midline cleft abnormality analyzed by whole exome sequencing. Known pathogenic homozygous variant c.2908C > T; (p.Arg970Ter) in exon 26 of COL18A1 was found as a cause for KS. These two siblings presented with early-onset severe ocular manifestations, facial dysmorphism, and variable central nervous system manifestations along with novel cerebellar midline cleft abnormality. The presence or absence of structural brain malformations and genotypes does not absolutely predict cognitive functions in KS patients. However, the presence of posterior fossa abnormality may be predictive for the development of ataxia in later life and needs further studies.

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期刊介绍: The Journal of Pediatric Genetics is an English multidisciplinary peer-reviewed international journal publishing articles on all aspects of genetics in childhood and of the genetics of experimental models. These topics include clinical genetics, molecular genetics, biochemical genetics, medical genetics, dysmorphology, teratology, genetic counselling, genetic engineering, formal genetics, neuropsychiatric genetics, behavioral genetics, community genetics, cytogenetics, hereditary or syndromic cancer genetics, genetic mapping, reproductive genetics, fetal pathology and prenatal diagnosis, multiple congenital anomaly syndromes, and molecular embryology of birth defects. Journal of Pediatric Genetics provides an in-depth update on new subjects and current comprehensive coverage of the latest techniques used in the diagnosis of childhood genetics. Journal of Pediatric Genetics encourages submissions from all authors throughout the world. The following articles will be considered for publication: editorials, original and review articles, short report, rapid communications, case reports, letters to the editor, and book reviews. The aim of the journal is to share and disseminate knowledge between all disciplines in the field of pediatric genetics. This journal is a publication of the World Pediatric Society: http://www.worldpediatricsociety.org/ The Journal of Pediatric Genetics is available in print and online. Articles published ahead of print are available via the eFirst service on the Thieme E-Journals platform.
期刊最新文献
Erratum: Corrigendum: A Severe Case of Spondylometaphyseal Dysplasia Algerian Type with Two Mutations in COL2A1. Microdeletion 3q13.33-3q21.2: A Rare Cause of Neurodevelopmental Disorder. Understanding the Endocrine and Molecular Signaling Cascade Regulation Pathways in Children with Hypospadias. A Rare Case of Neuronal Ceroid Lipofuscinosis-Type 1 (NCL-1) with Vitamin D-Dependent Rickets-Type 1 (VDDR-1), Complex 1 Mitochondrial Deficiency, and Mixed Variant-Checkerboard and Phylloid Type of Pigmentary Mosaicism. Contributing Reviewers in 2023.
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