Recessive HYDIN Mutations Cause Primary Ciliary Dyskinesia without Randomization of Left-Right Body Asymmetry

Olbrich, Heike; Schmidts, Miriam; Werner, Claudius; Onoufriadis, Alexandros; Loges, Niki T.; Raidt, Johanna; Bánki, Nóra Fanni; Shoemark, Amelia; Burgoyne, Thomas; Turki, Saeed Al; Hurles, Matthew E.; Köhler, Gabriele; Schroeder, Josef; Nürnberg, Gudrun; Nürnberg, Peter; Chung, Eddie M.K.; Reinhardt, Richard; Marthin, June Kehlet; Nielsen, Kim G.; Mitchison, Hannah M.; Omran, Heymut

doi:10.1016/j.ajhg.2012.08.016

Cited by 253 publications

(221 citation statements)

References 56 publications

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“…While tremendous progress has been made in recent years in unveiling the molecular mechanisms of the disease [2,3,[8][9][10][11][12][13][14][15][16][17][18][19], PCD management is still hampered by a lack of fundamental data on epidemiology, clinical presentation, disease course and effects of different treatment strategies [4][5][6]. Patient registries are well-known tools to assemble sufficient numbers of individuals with a rare disease to assess and monitor patient data in a standardised and longitudinal way, and to recruit candidates for clinical research studies [20,21].…”

Section: Introductionmentioning

confidence: 99%

An international registry for primary ciliary dyskinesia

et al. 2015

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Primary ciliary dyskinesia (PCD) is a rare autosomal recessive disorder leading to chronic upper and lower airway disease. Fundamental data on epidemiology, clinical presentation, course and treatment strategies are lacking in PCD. We have established an international PCD registry to realise an unmet need for an international platform to systematically collect data on incidence, clinical presentation, treatment and disease course.The registry was launched in January 2014. We used internet technology to ensure easy online access using a web browser under www.pcdregistry.eu. Data from 201 patients have been collected so far. The database is comprised of a basic data form including demographic and diagnostic information, and visit forms designed to monitor the disease course.To establish a definite PCD diagnosis, we used strict diagnostic criteria, which required two to three diagnostic methods in addition to classical clinical symptoms. Preliminary analysis of lung function data demonstrated a mean annual decline of percentage predicted forced expiratory volume in 1 s of 0.59% (95% CI 0.98-0.22).Here, we present the development of an international PCD registry as a new promising tool to advance the understanding of this rare disorder, to recruit candidates for research studies and ultimately to improve PCD care. @ERSpublications A registry to systematically collect data on clinical presentation, disease course and treatment of PCD http://ow.ly/TtGAR

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Section: Introductionmentioning

confidence: 99%

An international registry for primary ciliary dyskinesia

et al. 2015

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“…Studies have shown that mutations in genes affecting the central pair of microtubules can cause laterality abnormalities while mutations in genes affecting portions of the cilia other than the central pair do not affect laterality. 65,66 It is not only flow of embryonic fluid created by this rotary movement of cilia that affects laterality, however, but also impairment in ciliary sensory function. While the motile nodal cilia create the leftward flow of embryonic fluid, there is the requirement of downstream cilia to sense the flow, thus producing the co-called two-cilia hypothesis.…”

Section: Discussionmentioning

confidence: 99%

Genetic Disturbances in Patients with Bodily Isomerism from a Single Center: Clinical Implications of Affected Genes and Potential Impact of Ciliary Dyskinesia

Loomba

Frommelt

Anderson³

2016

Cardiogenetics

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So-called heterotaxy or isomerism is characterized by abnormal lateralization and malformations of the bodily organs. The mechanism is unclear, although there is growing evidence that ciliary dyskinesia is involved. We reviewed genetic findings from patients with isomerism to determine if affected genes were known to be associated with isomerism and ciliary dyskinesia and determine associations between genotype and clinical findings. We identified patients with isomerism cared for over a 16-year period. Characteristics were compared between those with and without identified mutations. A total of 83 patients with isomerism were identified. Of those who had genotyping, 14/27 had mutations identified, most frequently involving the CFC1 and NODAL genes. Specific mutations were associated with clinical findings, with NODAL mutations often portending need for increased clinical support. Genes associated with isomerism and/or ciliary dyskinesia were identified in the cohort. Specific gene mutations may help predict clinical course.

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“…For example, defects of nexin link components [63], central pair components [64], ciliary biogenesis defects [14] and defects caused by DNAH11 [65,66], usually cannot be visualized by classic TEM. Thus, normal ultrastructure cannot rule out PCD.…”

Section: Page 5 Of 36mentioning

confidence: 99%

“…Male patients with mutations in CCDC114 (coding for a docking protein for the ODA) are generally fertile [70]. Situs abnormalities are not observed in patients with mutations affecting the central pair [64] or radial spokes [49,50,69], nor in patients with reduced generation of multiple motile cilia [13,14]. However, it is likely that variable clinical pictures occur between patients with different mutations within a particular gene and even between patients with identical mutations.…”

Section: Genetics: Pcd Is Generally An Autosomal Recessive Disease Tmentioning

confidence: 99%

Diagnostic Methods in Primary Ciliary Dyskinesia

Lucas

Paff

Goggin

et al. 2016

Paediatric Respiratory Reviews

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Educational Aims; The reader will be able to; Describe the basis of the various diagnostic tests for PCD  Have an understanding of the strengths and limitations of each test  Understand that there is no 'gold standard' test  Understand why highly specialised centres should analyse samples and interpret results. Page 2 of 36A c c e p t e d M a n u s c r i p t  SummaryDiagnosing primary ciliary dyskinesia is difficult. With no reference standard, a combination of tests is needed; most tests require expensive equipment and specialist scientists. We review the advances in diagnostic testing over the past hundred years, with emphasis on recent advances.We particularly focus on use of high-speed video analysis, transmission electron microscopy, nasal nitric oxide and genetic testing. We discuss the international efforts that are in place to advance the evidence base for diagnostic tests.

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Recessive HYDIN Mutations Cause Primary Ciliary Dyskinesia without Randomization of Left-Right Body Asymmetry

Cited by 253 publications

References 56 publications

An international registry for primary ciliary dyskinesia

An international registry for primary ciliary dyskinesia

Genetic Disturbances in Patients with Bodily Isomerism from a Single Center: Clinical Implications of Affected Genes and Potential Impact of Ciliary Dyskinesia

Diagnostic Methods in Primary Ciliary Dyskinesia

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