A ciliopathy combining Joubert syndrome and Oro-Facial-Digital syndrome caused by bi-allelic 5'-UTR loss-of-function CEP83 variant.

IF 4.8 2区医学 Q1 GENETICS & HEREDITY

NPJ Genomic Medicine Pub Date : 2025-10-10 DOI:10.1038/s41525-025-00514-3

Matan M Jean, Anan Yunis, Tzofit Elbaz-Biton, Vadim Dolgin, Ginat Narkis, Analia Michaelovsky, Marina Eskin-Schwartz, Alexandra A Tsitrina, Nadav Agam, Tomer Poleg, Amit Safran, Ofek Freund, Noam Hadar, Dan Levy, Ilan Shelef, Khalil El Amour, Hagit Flusser, Ohad S Birk

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引用次数: 0

Abstract

Oro-Facial-Digital Syndrome (OFDS) and Joubert syndrome are ciliary disorders. Fifteen individuals of consanguineous Bedouin kindred presented with global developmental delay with no speech, and a clear OFDS phenotype, combined with Joubert syndrome, with MRI showing hypoplastic corpus callosum and molar tooth sign. Renal and liver function tests and ultrasound were unremarkable. Within a 0.5 Mb disease-associated locus (LOD score 6.2), whole genome sequencing identified a single variant: CEP83 NG_051825.2:g.5774dupG, (NM_016122.3):c.-278dupG. Patient fibroblasts showed aberrantly long cilia, and alternative splicing of CEP83 5'UTR, skipping most of exon 1 of the canonical transcript, and frameshift, abrogating CEP83 mRNA and protein expression. CEP83 acts in primary cilium assembly. CEP83 biallelic missense or in-frame deletions, with presumed residual function, were previously associated with early-onset nephronophthisis culminating in end-stage renal disease. We now demonstrate that a biallelic complete loss-of-function CEP83 variant culminates in elongated primary cilia, causing OFDS with Joubert-like features without evident renal involvement.

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由双等位基因5′-UTR功能丧失CEP83变异引起的Joubert综合征和Oro-Facial-Digital综合征合并纤毛病。

oro - face - digital Syndrome （OFDS）和Joubert综合征是纤毛疾病。15例贝都因近亲表现为全面发育迟缓，无言语，明显的OFDS表型，合并Joubert综合征，MRI显示胼胝体发育不全和磨牙征。肾、肝功能检查及超声检查无明显异常。在0.5 Mb的疾病相关位点（LOD评分6.2）中，全基因组测序鉴定出单个变异：CEP83 NG_051825.2:g。5774 dupg (NM_016122.3): c - 278 dupg。患者成纤维细胞表现出异常长的纤毛，CEP83 5'UTR的选择性剪接，跳过了规范转录物的大部分外显子1，以及移码，取消了CEP83 mRNA和蛋白的表达。CEP83在初级纤毛大会上起作用。CEP83双等位基因错义或框架内缺失，假定有残余功能，以前与早发性肾肾病相关，最终导致终末期肾病。我们现在证明，双等位基因完全功能丧失的CEP83变体最终导致初级纤毛延长，导致具有joubert样特征的OFDS，但没有明显的肾脏受累。

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

NPJ Genomic Medicine Biochemistry, Genetics and Molecular Biology-Molecular Biology

CiteScore

9.40

自引率

1.90%

发文量

审稿时长

17 weeks

期刊介绍： npj Genomic Medicine is an international, peer-reviewed journal dedicated to publishing the most important scientific advances in all aspects of genomics and its application in the practice of medicine. The journal defines genomic medicine as "diagnosis, prognosis, prevention and/or treatment of disease and disorders of the mind and body, using approaches informed or enabled by knowledge of the genome and the molecules it encodes." Relevant and high-impact papers that encompass studies of individuals, families, or populations are considered for publication. An emphasis will include coupling detailed phenotype and genome sequencing information, both enabled by new technologies and informatics, to delineate the underlying aetiology of disease. Clinical recommendations and/or guidelines of how that data should be used in the clinical management of those patients in the study, and others, are also encouraged.