| Literature DB >> 27637300 |
Francesca Boaretto1, Deborah Snijders2, Cecilia Salvoro1, Ambra Spalletta1, Maria Luisa Mostacciuolo1, Mirella Collura3, Salvatore Cazzato4, Donatella Girosi5, Michela Silvestri5, Giovanni Arturo Rossi5, Angelo Barbato2, Giovanni Vazza6.
Abstract
Primary ciliary dyskinesia (PCD) is a rare genetic disorder that alters mucociliary clearance, with consequent chronic disease of upper and lower airways. Diagnosis of PCD is challenging, and genetic testing is hampered by the high heterogeneity of the disease, because autosomal recessive causative mutations were found in 34 different genes. In this study, we clinically and molecularly characterized a cohort of 51 Italian patients with clinical signs of PCD. A custom next-generation sequencing panel that enables the affordable and simultaneous screening of 24 PCD genes was developed for genetic analysis. After variant filtering and prioritization, the molecular diagnosis of PCD was achieved in 43% of the patients. Overall, 5 homozygous and 27 compound heterozygous mutations, 21 of which were never reported before, were identified in 11 PCD genes. The DNAH5 and DNAH11 genes were the most common cause of PCD in Italy, but some population specificities were identified. In addition, the number of unsolved cases and the identification of only a single mutation in six patients suggest further genetic heterogeneity and invoke the need of novel strategies to detect unconventional pathogenic DNA variants. Finally, despite the availability of mutation databases and in silico prediction tools helping the interpretation of variants in next-generation sequencing screenings, a comprehensive segregation analysis is required to establish the in trans inheritance and support the pathogenic role of mutations.Entities:
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Year: 2016 PMID: 27637300 DOI: 10.1016/j.jmoldx.2016.07.002
Source DB: PubMed Journal: J Mol Diagn ISSN: 1525-1578 Impact factor: 5.568