Novel Gene Variants Associated with Primary Ciliary Dyskinesia

Durkadin Demir Eksi; Elanur Yilmaz; A Erdem Basaran; Gizem Erduran; Banu Nur; Ercan Mihci; Bulent Karadag; Aysen Bingol; Ozgul M Alper

doi:10.1007/s12098-022-04098-z

Novel Gene Variants Associated with Primary Ciliary Dyskinesia

Indian J Pediatr. 2022 Jul;89(7):682-691. doi: 10.1007/s12098-022-04098-z. Epub 2022 Mar 3.

Authors

Durkadin Demir Eksi^{1

2}, Elanur Yilmaz^{3

4}, A Erdem Basaran⁵, Gizem Erduran³, Banu Nur⁶, Ercan Mihci⁶, Bulent Karadag⁷, Aysen Bingol⁵, Ozgul M Alper⁸

Affiliations

¹ Department of Medical Biology and Genetics, School of Medicine, Akdeniz University, Antalya, 07070, Turkey. durkadin.eksi@alanya.edu.tr.
² Department of Medical Biology, School of Medicine, Alanya Alaaddin Keykubat University, Antalya, 07425, Turkey. durkadin.eksi@alanya.edu.tr.
³ Department of Medical Biology and Genetics, School of Medicine, Akdeniz University, Antalya, 07070, Turkey.
⁴ Department of Medical Genetics & Koç University Research Center for Translational Medicine (KUTTAM), School of Medicine, Koç University, Istanbul, Turkey.
⁵ Department of Pediatric Pulmonology, School of Medicine, Akdeniz University, Antalya, Turkey.
⁶ Department of Pediatric Genetics, School of Medicine, Akdeniz University, Antalya, Turkey.
⁷ Department of Pediatric Pulmonology, School of Medicine, Marmara University, Istanbul, Turkey.
⁸ Department of Medical Biology and Genetics, School of Medicine, Akdeniz University, Antalya, 07070, Turkey. oalper@akdeniz.edu.tr.

PMID: 35239159
DOI: 10.1007/s12098-022-04098-z

Abstract

Objectives: To determine the demographic, clinical, and genetic profile of Turkish Caucasian PCD cases.

Methods: Targeted next-generation sequencing (t-NGS) of 46 nuclear genes was performed in 21 unrelated PCD cases. Sanger sequencing confirmed of potentially disease-related variations, and genotype-phenotype correlations were evaluated.

Results: Disease-related variations were identified in eight different genes (CCDC39, CCDC40, CCDC151, DNAAF2, DNAAF4, DNAH11, HYDIN, RSPH4A) in 52.4% (11/21) of the cases. The frequency of variations for CCDC151, DNAH11, and DNAAF2 genes which were highly mutated genes in the cohort was 18% in 11 patients. Each of the remaining gene variations was detected once (9%) in different patients. The variants, p.R482fs*12 in CCDC151, p.E216* in DNAAF2, p.I317* in DNAAF4, p.L318P and p.R1865* in DNAH11, and p.N1505D and p.L1167P in HYDIN gene were identified as novel variations. Interestingly, varying phenotypic findings were identified even in patients with the same mutation, which once again confirmed that PCD has a high phenotypic heterogeneity and shows individual differences.

Conclusion: This t-NGS panel is potentially helpful for exact and rapid identification of reported/novel PCD-disease-causing variants to establish the molecular diagnosis of ciliary diseases.

Keywords: Ciliary diseases; Mutation analysis; Primary ciliary dyskinesia; Targeted next-generation sequencing.

MeSH terms

Cohort Studies
Genetic Association Studies
High-Throughput Nucleotide Sequencing
Humans
Kartagener Syndrome* / diagnosis
Kartagener Syndrome* / genetics
Mutation