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Literature DB >> 31545650

SPEF2- and HYDIN-Mutant Cilia Lack the Central Pair-associated Protein SPEF2, Aiding Primary Ciliary Dyskinesia Diagnostics.

Sandra Cindrić¹, Gerard W Dougherty¹, Heike Olbrich¹, Rim Hjeij¹, Niki Tomas Loges¹, Israel Amirav², Maria C Philipsen³, June K Marthin³, Kim G Nielsen³, Sivagurunathan Sutharsan⁴, Johanna Raidt¹, Claudius Werner⁵, Petra Pennekamp¹, Bernd Dworniczak¹, Heymut Omran¹.

Abstract

Primary ciliary dyskinesia (PCD) is a genetically heterogeneous chronic destructive airway disease. PCD is traditionally diagnosed by nasal nitric oxide measurement, analysis of ciliary beating, transmission electron microscopy (TEM), and/or genetic testing. In most genetic PCD variants, laterality defects can occur. However, it is difficult to establish a diagnosis in individuals with PCD and central pair (CP) defects, and alternative strategies are required because of very subtle ciliary beating abnormalities, a normal ciliary ultrastructure, and normal situs composition. Mutations in HYDIN are known to cause CP defects, but the genetic analysis of HYDIN variants is confounded by the pseudogene HYDIN2, which is almost identical in terms of intron/exon structure. We have previously shown that several types of PCD can be diagnosed via immunofluorescence (IF) microscopy analyses. Here, using IF microscopy, we demonstrated that in individuals with PCD and CP defects, the CP-associated protein SPEF2 is absent in HYDIN-mutant cells, revealing its dependence on functional HYDIN. Next, we performed IF analyses of SPEF2 in respiratory cells from 189 individuals with suspected PCD and situs solitus. Forty-one of the 189 individuals had undetectable SPEF2 and were subjected to a genetic analysis, which revealed one novel loss-of-function mutation in SPEF2 and three reported and 13 novel HYDIN mutations in 15 individuals. The remaining 25 individuals are good candidates for new, as-yet uncharacterized PCD variants that affect the CP apparatus. SPEF2 mutations have been associated with male infertility but have not previously been identified to cause PCD. We identified a mutation of SPEF2 that is causative for PCD with a CP defect. We conclude that SPEF2 IF analyses can facilitate the detection of CP defects and evaluation of the pathogenicity of HYDIN variants, thus aiding the molecular diagnosis of CP defects.

Entities: Disease Gene

Keywords: HYDIN2; cilia; immunofluorescence microscopy analysis; situs solitus; test sensitivity and specificity

Year: 2020 PMID： 31545650 DOI： 10.1165/rcmb.2019-0086OC

Source DB: PubMed Journal: Am J Respir Cell Mol Biol ISSN： 1044-1549 Impact factor: 6.914

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6. The global prevalence and ethnic heterogeneity of primary ciliary dyskinesia gene variants: a genetic database analysis.

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SPEF2- and HYDIN-Mutant Cilia Lack the Central Pair-associated Protein SPEF2, Aiding Primary Ciliary Dyskinesia Diagnostics.

1. Ciliary central apparatus structure reveals mechanisms of microtubule patterning.

2. Clinical and Genetic Spectrum of Children With Primary Ciliary Dyskinesia in China.

3. Update in Pediatrics 2020.

4. Chlamydomonas FAP70 is a component of the previously uncharacterized ciliary central apparatus projection C2a.

5. Sperm flagellar 2 (SPEF2) is essential for sperm flagellar assembly in humans.

6. The global prevalence and ethnic heterogeneity of primary ciliary dyskinesia gene variants: a genetic database analysis.

7. HY-DIN' in the Cilia: Discovery of Central Pair-related Mutations in Primary Ciliary Dyskinesia.

Review 8. Motile cilia genetics and cell biology: big results from little mice.

Review 9. Emerging Genotype-Phenotype Relationships in Primary Ciliary Dyskinesia.

Review 10. Rare Human Diseases: Model Organisms in Deciphering the Molecular Basis of Primary Ciliary Dyskinesia.