AI Article Synopsis
- Primary ciliary dyskinesia (PCD) is a complex disorder with a narrow range of symptoms, making diagnosis difficult due to its similarities with other conditions and reliance on specialized tests.
- In a study involving 81 patients with suspected PCD, exome sequencing revealed that 68% had identifiable genetic variants linked to PCD, with common symptoms including sinus and lung infections.
- The research also identified new potential gene candidates and noted instances where other genetic variants caused similar symptoms, highlighting the utility of exome sequencing in making PCD diagnosis more accessible.
Article Abstract
Unlike disorders of primary cilium, primary ciliary dyskinesia (PCD) has a much narrower clinical spectrum consistent with the limited tissue distribution of motile cilia. Nonetheless, PCD diagnosis can be challenging due to the overlapping features with other disorders and the requirement for sophisticated tests that are only available in specialized centers. We performed exome sequencing on all patients with a clinical suspicion of PCD but for whom no nasal nitric oxide test or ciliary functional assessment could be ordered. Among 81 patients (56 families), in whom PCD was suspected, 68% had pathogenic or likely pathogenic variants in established PCD-related genes that fully explain the phenotype (20 variants in 11 genes). The major clinical presentations were sinopulmonary infections (SPI) (n = 58), neonatal respiratory distress (NRD) (n = 2), laterality defect (LD) (n = 6), and combined LD/SPI (n = 15). Biallelic likely deleterious variants were also encountered in AKNA and GOLGA3, which we propose as novel candidates in a lung phenotype that overlaps clinically with PCD. We also encountered a PCD phenocopy caused by a pathogenic variant in ITCH, and a pathogenic variant in CEP164 causing Bardet-Biedl syndrome and PCD presentation as a very rare example of the dual presentation of these two disorders of the primary and motile cilia. Exome sequencing is a powerful tool that can help "democratize" the diagnosis of PCD, which is currently limited to highly specialized centers.
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| http://dx.doi.org/10.1007/s00439-020-02170-2 | DOI Listing |
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