Characterization of a novel deep-intronic variant in DYNC2H1 identified by whole-exome sequencing in a patient with a lethal form of a short-rib thoracic dysplasia type III

Characterization of a novel deep-intronic variant in DYNC2H1 identified by whole-exome sequencing in a patient with a lethal form of a short-rib thoracic dysplasia type III

Biallelic pathogenic variants in are the cause of short-rib thoracic dysplasia type III with or without polydactyly (OMIM #613091), a skeletal ciliopathy characterized by thoracic hypoplasia due to short ribs. In this report, we review the case of a patient who was admitted to the Neonatal Intensive...

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Veröffentlicht in:Cold Spring Harbor molecular case studies 2022-12, Vol.8 (7), p.a006254
Hauptverfasser: Buchh, Muqsit, Gillespie, Patrick J, Treat, Kayla, Abreu, Marco A, Schwantes-An, Tae-Hwi Linus, Helm, Benjamin M, Fang, Fang, Xuei, Xiaoling, Mantcheva, Lili, Suhrie, Kristen R, Graham, Brett H, Conboy, Erin, Vetrini, Francesco
Format: Artikel
Sprache:eng
Schlagworte:
Bones
Cytoplasmic Dyneins - genetics
Diagnosis
DNA microarrays
Dysplasia
Exome Sequencing
Female
Fibroblasts
Gene sequencing
Genetic screening
Humans
Hypoplasia
Infant, Newborn
Lung diseases
mRNA turnover
Mutation
Neonates
Nonsense mutation
Nonsense-mediated mRNA decay
Pathogenicity
Pathogens
Polydactyly
Pregnancy
Rib
Ribs
RNA, Messenger
Short Rib-Polydactyly Syndrome - diagnosis
Short Rib-Polydactyly Syndrome - genetics
Splicing
Stop codon
Thorax
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Zusammenfassung:Biallelic pathogenic variants in are the cause of short-rib thoracic dysplasia type III with or without polydactyly (OMIM #613091), a skeletal ciliopathy characterized by thoracic hypoplasia due to short ribs. In this report, we review the case of a patient who was admitted to the Neonatal Intensive Care Unit (NICU) of Indiana University Health (IUH) for respiratory support after experiencing respiratory distress secondary to a small, narrow chest causing restrictive lung disease. Additional phenotypic features include postaxial polydactyly, short proximal long bones, and ambiguous genitalia were noted. Exome sequencing (ES) revealed a maternally inherited likely pathogenic variant c.10322C > T p.(Leu3448Pro) in the gene. However, there was no variant found on the paternal allele. Microarray analysis to detect deletion or duplication in was normal. Therefore, there was insufficient evidence to establish a molecular diagnosis. To further explore the data and perform additional investigations, the patient was subsequently enrolled in the Undiagnosed Rare Disease Clinic (URDC) at Indiana University School of Medicine (IUSM). The investigators at the URDC performed a reanalysis of the ES raw data, which revealed a paternally inherited deep-intronic variant c.10606-14A > G predicted to create a strong cryptic acceptor splice site. Additionally, the RNA sequencing of fibroblasts demonstrated partial intron retention predicted to cause a premature stop codon and nonsense-mediated mRNA decay (NMD). Droplet digital RT-PCR (RT-ddPCR) showed a drastic reduction by 74% of mRNA levels. As a result, the intronic variant was subsequently reclassified as likely pathogenic resulting in a definitive clinical and genetic diagnosis for this patient. Reanalysis of ES and fibroblast mRNA experiments confirmed the pathogenicity of the splicing variants to supplement critical information not revealed in original ES or CMA reports. The NICU and URDC collaboration ended the diagnostic odyssey for this family; furthermore, its importance is emphasized by the possibility of prenatally diagnosing the mother's current pregnancy.
ISSN:2373-2865
2373-2873
DOI:10.1101/mcs.a006254