Abstract
Primary ciliary dyskinesia (PCD) is a rare autosomal recessive disorder with defective structure and/or function of motile cilia/flagella, causing chronic upper and lower respiratory tract infections, fertility problems, and disorders of organ laterality. Diagnosing PCD requires a combined approach utilizing characteristic phenotypes and complementary methods for detection of defects of ciliary function and ultrastructure, measurement of nasal nitric oxide and genetic testing. Currently, biallelic mutations in 31 different genes have been linked to PCD allowing a genetic diagnosis in approximately ~ 60% of cases. Management includes surveillance of pulmonary function, imaging, and microbiology of upper and lower airways in addition to daily airway clearance and prompt antibiotic treatment of infections. Early referral to specialized centers that use a multidisciplinary approach is likely to improve outcomes. Currently, evidence-based knowledge on PCD care is missing let alone management guidelines. Research and clinical investigators, supported by European and North American patient support groups, have joined forces under the name of BESTCILIA, a European Commission funded consortium dedicated to improve PCD care and knowledge. Core programs of this network include the establishment of an international PCD registry, the generation of disease specific PCD quality of life questionnaires, and the first randomized controlled trial in PCD.
Highlights
Primary ciliary dyskinesia (PCD) is a rare autosomal recessive disorder with defective structure and/or function of motile cilia/flagella, causing chronic upper and lower respiratory tract infections, fertility problems, and disorders of organ laterality
Subsequent research lead to the replacement of the term ‘immotile cilia syndrome’ by ‘primary ciliary dyskinesia’ in order to emphasize that ciliary immotility and abnormal ciliary motility causes PCD [2]. Even this term seems to be inappropriate to cover all disease variants, as demonstrated by the recent identification of a disease entity characterized by typical, severe clinical PCD features caused by defective generation of multiple motile cilia [3,4]
This review provides a state-of-the art overview on diagnosis and management of PCD
Summary
Individuals with both upper and lower respiratory tract disease a. Upper airways disease includes: chronic rhinitis/nasal discharge, chronic sinusitis, hearing impairment due to glue ear, chronic otitis media b. Lower airways disease includes: chronic wet cough, atelectasis or bronchiectasis, notably in middle lobe, lingula or lower lobes, chronic/recurrent bronchitis/pneumonia
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