Identification of a Novel Nonsense Variant in the DLL3 Gene Underlying Spondylocostal Dysostosis in a Consanguineous Pakistani Family

Feroz Khan; Abida Arshad; Asmat Ullah; Ellen Steenackers; Geert Mortier; Wasim Ahmad; Muhammad Arshad; Sarmir Khan; Amir Hayat; Ikram Khan; Muhammad Asim Khan; Wim Van Hul

doi:10.1159/000527043

Identification of a Novel Nonsense Variant in the DLL3 Gene Underlying Spondylocostal Dysostosis in a Consanguineous Pakistani Family

Mol Syndromol. 2023 Jun;14(3):191-200. doi: 10.1159/000527043. Epub 2023 Feb 1.

Authors

Feroz Khan^{1

2

3}, Abida Arshad¹, Asmat Ullah⁴, Ellen Steenackers², Geert Mortier², Wasim Ahmad⁴, Muhammad Arshad⁵, Sarmir Khan⁶, Amir Hayat⁷, Ikram Khan⁸, Muhammad Asim Khan⁹, Wim Van Hul²

Affiliations

¹ Department of Zoology, Wild Life and Fisheries, Pir Mehr Ali Shah Arid Agriculture University, Rawalpindi, Pakistan.
² Department of Medical Genetics, University of Antwerp, Antwerp, Belgium.
³ Department of Zoology, University of Science and Technology, Bannu, Pakistan.
⁴ Department of Biochemistry, Faculty of Biological Sciences, Quaid-i-Azam University, Islamabad, Pakistan.
⁵ Department of Biological Sciences, International Islamic University, Islamabad, Pakistan.
⁶ Department of Reproductive Medicine, Academy of Medical Sciences, The First Affiliated Hospital of Zhengzhou University, Zhengzhou, China.
⁷ Department Biochemistry, Faculty of Life and Chemical Sciences, Abdul Wali Khan University, Mardan, Pakistan.
⁸ School of Life Sciences, Lanzhou University, Lanzhou, China.
⁹ Department of Zoology, Faculty of Biological Sciences, Quaid-i-Azam University, Islamabad, Pakistan.

Abstract

Introduction: Spondylocostal dysostosis (SCD) is characterized by multiple vertebral abnormalities associated with abnormalities of the ribs. Five genes causative for the disease have been identified. These include DLL3 (OMIM *602768), MESP2 (OMIM #608681), LFNG (OMIM #609813), TBX6 (OMIM *602427), and HES7 (OMIM *608059).

Methods: In the current study, we investigated a Pakistani consanguineous family segregating spondylocostal dysotosis. Whole-exome sequencing (WES) followed by Sanger sequencing was performed using DNA of affected and unaffected individuals to identify pathogenic variant(s). The identified variant was interpreted using ACMG classification. Literature review was performed to summarize currently known mutated alleles of DLL3 and the underlying clinical phenotypes.

Results: Clinical examination using anthropometric measurements and radiographs diagnosed the patients to be afflicted with SCD. Pedigree analysis of the affected family showed an autosomal recessive inheritance pattern of the disease. WES followed by Sanger sequencing identified a novel homozygous nonsense variant (DLL3(NM_016941.4): c.535G>T; p.Glu179Ter) in the DLL3 gene located on chromosome 19q13.2.

Conclusion: The study will be helpful in carrier testing and genetic counseling to prevent segregation of the disease to the next generations within this family. It also provides knowledge for clinicians and researchers in search of a better understanding of SCD anomalies.

Keywords: DLL3; Novel nonsense variant; Spondylocostal dysostosis; Whole-exome sequencing.

Grants and funding

This work was funded by the higher education commission (HEC) Pakistan on the basis of International Research Supportive Initiative Program (IRSIP) to Feroz Khan. Genetic analysis of the family was done at the Department of Medical Genetics, University of Antwerp, Belgium.