Prevalence of primary ciliary dyskinesia in consecutive referrals of suspect cases and the transmission electron microscopy detection rate: a systematic review and meta-analysis

Kouis, Panayiotis; Yiallouros, Panayiotis Κ.; Middleton, Nicos; Evans, John S.; Kyriacou, Kyriacos; Papatheodorou, Stefania

doi:10.1038/pr.2016.263

Cited by 48 publications

(52 citation statements)

References 51 publications

(88 reference statements)

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“…Current estimates suggest that approximately 30% of PCD cases have normal or non-diagnostic ciliary ultrastructure, 1,2 and a recent meta-analysis reports at least 26% of PCD, diagnosed through genetics, HSVA, or nasal nitric oxide measurement, lack detectable ultrastructural changes on TEM. 3 Therefore, clinicians cannot conclude that a normal TEM analysis excludes PCD. Respiratory viral infections, environmental pollutants and other airway insults can induce secondary changes in ciliary ultrastructure that may overlap with some of the subtle changes seen in PCD; therefore, care must be taken to avoid misinterpretation of these secondary changes as “consistent with PCD”.…”

Section: Introductionmentioning

confidence: 99%

Value of transmission electron microscopy for primary ciliary dyskinesia diagnosis in the era of molecular medicine: Genetic defects with normal and non-diagnostic ciliary ultrastructure

Shapiro

Leigh

2017

Ultrastructural Pathology

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Primary Ciliary Dyskinesia (PCD) is a genetic disorder causing chronic oto-sino-pulmonary disease. No single diagnostic test will detect all PCD cases. Transmission electron microscopy (TEM) of respiratory cilia was previously considered the gold standard diagnostic test for PCD, but 30% of all PCD cases have either normal ciliary ultrastructure or subtle changes which are non-diagnostic. These cases are identified through alternate diagnostic tests, including nasal nitric oxide measurement, high speed videomicroscopy analysis, immunofluorescent staining of axonemal proteins, and/or mutation analysis of various PCD causing genes. Autosomal recessive mutations in DNAH11 and HYDIN produce normal TEM ciliary ultrastructure, while mutations in genes encoding for radial spoke head proteins result in some cross-sections with non-diagnostic alterations in the central apparatus interspersed with normal ciliary cross-sections. Mutations in nexin link and dynein regulatory complex genes lead to a collection of different ciliary ultrastructures; mutations in CCDC65, CCDC164, and GAS8 produce normal ciliary ultrastructure, while mutations in CCDC39 and CCDC40 cause absent inner dynein arms and microtubule disorganization in some ciliary cross-sections. Mutations in CCNO and MCIDAS cause near complete absence of respiratory cilia due to defects in generation of multiple cellular basal bodies; however, the scant cilia generated may have normal ultrastructure. Lastly, a syndromic form of PCD with retinal degeneration results in normal ciliary ultrastructure through mutations in the RPGR gene. Clinicians must be aware of these genetic causes of PCD resulting in non-diagnostic TEM ciliary ultrastructure and refrain from using TEM of respiratory cilia as a test to rule out PCD.

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Section: Introductionmentioning

confidence: 99%

Value of transmission electron microscopy for primary ciliary dyskinesia diagnosis in the era of molecular medicine: Genetic defects with normal and non-diagnostic ciliary ultrastructure

Shapiro

Leigh

2017

Ultrastructural Pathology

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“…We used a modern reference standard diagnosis for PCD based on widely available clinical tests (cilia TEM, genetics, and nasal nitric oxide) and sensitivity analyses removing the nasal nitric oxide criteria did not change the results. Ciliary ultrastructural analysis by TEM is normal or nondiagnostic in 30% to 50% of patients with PCD and current genetic testing detects only 65% to 70% of PCD cases . Other tests to diagnose PCD, such as functional ciliary beat assessment via high‐speed video microscopy and immunofluorescence testing, also have limitations in feasibility and/or accuracy .…”

Section: Discussionmentioning

confidence: 99%

Evaluation of the pulmonary radioaerosol mucociliary clearance scan as an adjunctive test for the diagnosis of primary ciliary dyskinesia in children

Vali

Ghandourah

Charron³

et al. 2019

Pediatric Pulmonology

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Introduction The accuracy of primary ciliary dyskinesia (PCD) diagnosis has improved but no single test is diagnostic and some cases remain unsolved. Data regarding the accuracy of pulmonary radioaerosol mucociliary clearance scan (PRMCC) for the diagnosis of PCD are limited to predominantly adults using a 24‐hour test. This study was performed to determine the accuracy of a 60‐minute PRMCC test for diagnosing PCD in children. Methods Children with suspected PCD and inconclusive clinical diagnostic testing in an expert center were selected for PRMCC testing. Nebulized 99mTc sulfur colloid was inhaled and dynamic imaging acquired for 60 to 120 minutes. Two independent radiologists blinded to the clinical diagnosis and health records overread PRMCC studies. The PRMCC result was compared with the reference standard diagnosis of PCD made by two physicians using the cumulative health record, blinded to PRMCC results. Results From 2008 to 2018, 57 patients (6‐17 years) participated, of which 16 met criteria for the reference diagnosis of PCD. The PRMCC test was conclusive in 54 patients (94.7%) and had a sensitivity of 100% (95% confidence interval [CI] = 78.2–100), specificity of 85.7% (95% CI = 69.7–95.2), positive predictive value of 75% (95% CI = 57.1–87.1), negative predictive value of 100% (95% CI = 90.2–100), and accuracy of 90% (95% CI = 78.2–96.7). Conclusion The 60‐minute PRMCC test is noninvasive and feasible in children with a high negative predictive value for PCD. It may be a helpful adjunctive test to rule out PCD when clinical suspicion remains after guideline recommended first‐line clinical testing.

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“…In cases of suspected PCD in a patient with CRS since birth, a family history of PCD and/or associated features of Kartagener syndrome (situs inversus and infertility), one should consider diagnostic tests of ciliary function by evaluation of CBF, EM evaluation of the dynein arms of the cilia and/or evaluation of the cilia after ciliogenesis in vitro. In a tertiary referral centre, one third of patients referred with suspected PCD are eventually diagnosed with the condition (377) .…”

Section: Recommendationsmentioning

confidence: 99%

European position paper on diagnostic tools in rhinology

Rimmer

Hellings

Lund

et al. 2019

Rhin

114

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is the official Journal of the European and International Rhinologic Societies and appears quarterly in March, June, September and December. Cited in Pubmed, Current Contents, Index Medicus, Exerpta Medica and Embase Founded in 1963 by H.A.E. van Dishoeck, Rhinology is a worldwide non-profit making journal. The journal publishes original papers on basic research as well as clinical studies in the major field of rhinology, including physiology, diagnostics, pathology, immunology, medical therapy and surgery of both the nose and paranasal sinuses. Review articles and short communications are also pulished. All papers are peer-reviewed. Letters-to-the-editor provide a forum for comments on published papers, and are not subject to editorial revision except for correction of English language. In-depth studies that are too long to be included into a regular issue can be published as a supplement. Supple ments are not subject to peer-review.

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Prevalence of primary ciliary dyskinesia in consecutive referrals of suspect cases and the transmission electron microscopy detection rate: a systematic review and meta-analysis

Cited by 48 publications

References 51 publications

Value of transmission electron microscopy for primary ciliary dyskinesia diagnosis in the era of molecular medicine: Genetic defects with normal and non-diagnostic ciliary ultrastructure

Value of transmission electron microscopy for primary ciliary dyskinesia diagnosis in the era of molecular medicine: Genetic defects with normal and non-diagnostic ciliary ultrastructure

Evaluation of the pulmonary radioaerosol mucociliary clearance scan as an adjunctive test for the diagnosis of primary ciliary dyskinesia in children

European position paper on diagnostic tools in rhinology

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