An Example of the Utility of Genomic Analysis for Fast and Accurate Clinical Diagnosis of Complex Rare Phenotypes

Overview

Journal Orphanet J Rare Dis

Publisher Biomed Central

Specialty General Medicine

Date 2017 Feb 9

PMID 28173822

Citations 11

Authors

Polona Le Quesne Stabej

Chela James

Louise Ocaka

Mehmet Tekman

Stephanie Grunewald

Emma Clement

Horia C Stanescu

Robert Kleta

Deborah Morrogh

Alistair Calder

Hywel J Williams

Maria Bitner-Glindzicz

Affiliations

Soon will be listed here.

Abstract

Background: We describe molecular diagnosis in a complex consanguineous family: four offspring presented with combinations of three distinctive phenotypes; non-syndromic hearing loss (NSHL), an unusual skeletal phenotype comprising multiple fractures, cranial abnormalities and diaphyseal expansion, and significant developmental delay with microcephaly. We performed Chromosomal Microarray Analysis on the offspring with either the skeletal or developmental delay phenotypes, and linkage analysis and whole exome sequencing (WES) on all four children, parents and maternal aunt.

Results: Chromosomal microarray and FISH analysis identified a de novo unbalanced translocation as a cause of the microcephaly and severe developmental delay. WES identified a NSHL-causing splice variant in an autosomal recessive deafness gene PDZD7 which resided in a linkage region and affected three of the children. In the two children diagnosed with an unusual skeletal phenotype, WES eventually disclosed a heterozygous COL1A1 variant which affects C-propetide cleavage site of COL1. The variant was inherited from an apparently unaffected mosaic father in an autosomal dominant fashion. After the discovery of the COL1A1 variant, the skeletal phenotype was diagnosed as a high bone mass form of osteogenesis imperfecta.

Conclusions: Next generation sequencing offers an unbiased approach to molecular genetic diagnosis in highly heterogeneous and poorly characterised disorders and enables early diagnosis as well as detection of mosaicism.

Citing Articles

Clinical characterizations and molecular genetic study of two co-segregating variants in PDZD7 and PDE6C genes leading simultaneously to non-syndromic hearing loss and achromatopsia.

Nouri Z, Sarmadi A, Narrei S, Kianersi H, Kianersi F, Tabatabaiefar M BMC Med Genomics. 2024; 17(1):173.

PMID: 38956522 PMC: 11218353. DOI: 10.1186/s12920-024-01942-3.

Autosomal recessive non-syndromic hearing loss genes in Pakistan during the previous three decades.

Shadab M, Abbasi A, Ejaz A, Ben-Mahmoud A, Gupta V, Kim H J Cell Mol Med. 2024; 28(8):e18119.

PMID: 38534090 PMC: 10967143. DOI: 10.1111/jcmm.18119.

Rapid genome sequencing for pediatrics.

Jezkova J, Shaw S, Taverner N, Williams H Hum Mutat. 2022; 43(11):1507-1518.

PMID: 36086948 PMC: 9826377. DOI: 10.1002/humu.24466.

Novel homozygous variant in the PDZD7 gene in a family with nonsyndromic sensorineural hearing loss.

Du Q, Sun Q, Gu X, Wang J, Li W, Guo L BMC Med Genomics. 2022; 15(1):135.

PMID: 35715776 PMC: 9204979. DOI: 10.1186/s12920-022-01289-7.

High bone mass phenotype in a cohort of patients with Osteogenesis Imperfecta caused due to and C-propeptide cleavage variants in .

Campanini E, Baker D, Arundel P, Bishop N, Offiah A, Keigwin S Bone Rep. 2021; 15:101102.

PMID: 34277895 PMC: 8264105. DOI: 10.1016/j.bonr.2021.101102.

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