Your search keyword '"Maimoona A. Zariwala"' showing total 118 results

1. Primary Ciliary Dyskinesia: A Clinical Review

Author

Katherine A. Despotes, Maimoona A. Zariwala, Stephanie D. Davis, and Thomas W. Ferkol

Subjects

primary ciliary dyskinesia, cilia, motile ciliopathy, bronchiectasis, genotype, phenotype, Cytology, QH573-671

Abstract

Primary ciliary dyskinesia (PCD) is a rare, genetically heterogeneous, motile ciliopathy, characterized by neonatal respiratory distress, recurrent upper and lower respiratory tract infections, subfertility, and laterality defects. Diagnosis relies on a combination of tests for confirmation, including nasal nitric oxide (nNO) measurements, high-speed videomicroscopy analysis (HSVMA), immunofluorescent staining, axonemal ultrastructure analysis via transmission electron microscopy (TEM), and genetic testing. Notably, there is no single gold standard confirmatory or exclusionary test. Currently, 54 causative genes involved in cilia assembly, structure, and function have been linked to PCD; this rare disease has a spectrum of clinical manifestations and emerging genotype–phenotype relationships. In this review, we provide an overview of the structure and function of motile cilia, the emerging genetics and pathophysiology of this rare disease, as well as clinical features associated with motile ciliopathies, novel diagnostic tools, and updates on genotype–phenotype relationships in PCD.

Published

2024

2. Autosomal dominant variants in FOXJ1 causing primary ciliary dyskinesia in two patients with obstructive hydrocephalus

Author

Adam J. Shapiro, Kimberley Kaspy, M. Leigh Ann Daniels, Jaclyn R. Stonebraker, Van‐Hung Nguyen, Lyne Joyal, Michael R. Knowles, and Maimoona A. Zariwala

Subjects

Genetics, QH426-470

Abstract

Abstract Background Primary ciliary dyskinesia (PCD) is a mostly autosomal recessive, genetic disease of abnormal motile cilia function, resulting in bronchiectasis, infertility, organ laterality defects, and chronic otolaryngology disease. Though motile, ependymal cilia influencing cerebrospinal fluid flow in the central nervous system share many aspects of structure and function with motile cilia in the respiratory tract, hydrocephalus is rarely associated with PCD. Recently, pathogenic variants in FOXJ1 (Chr 17q25.1) were identified causing PCD associated with hydrocephalus, reduced respiratory cilia number, axonemal microtubule disorganization, and occurring in a de novo, autosomal dominant inheritance pattern. Method Two patients with chronic oto‐sino‐pulmonary disease and hydrocephalus underwent candidate testing of FOXJ1. Coding region and splice junctions were sequenced and analyzed under the auspices of Genetic Disorders of Mucociliary Clearance Consortium. Results Upon sequencing of the entire coding region and splice‐junctions, heterozygous, pathogenic variants in FOXJ1 were discovered in exon 3 of two patients: an 11‐month‐old female with situs inversus totalis (NM_001454.4: c.945delC (p.Phe315Leufs*18)) and a 51 year‐old male, post‐double lung transplantation (NM_001454.4: c.929_932delACTG (p.Asp310Glyfs*22)). FOXJ1 variants were not detected in the available parents and the siblings of these probands. Conclusion FOXJ1 pathogenic variants cause PCD in a de novo, autosomal dominant inheritance pattern, and are associated with hydrocephalus. Physicians treating patients with hydrocephalus and chronic oto‐sino‐pulmonary disease should be aware of this PCD association and test for FOXJ1 variants.

Published

2021

3. The expanding phenotype of OFD1‐related disorders: Hemizygous loss‐of‐function variants in three patients with primary ciliary dyskinesia

Author

William B. Hannah, Suzanne DeBrosse, BreAnna Kinghorn, Steven Strausbaugh, Moira L. Aitken, Margaret Rosenfeld, Whitney E. Wolf, Michael R. Knowles, and Maimoona A. Zariwala

Subjects

OFD1, Primary ciliary dyskinesia, Genetics, QH426-470

Abstract

Abstract Background OFD1 has long been recognized as the gene implicated in the classic dysmorphology syndrome, oral‐facial‐digital syndrome type I (OFDSI). Over time, pathogenic variants in OFD1 were found to be associated with X‐linked intellectual disability, Joubert syndrome type 10 (JBTS10), Simpson‐Golabi‐Behmel syndrome type 2 (SGBS2), and retinitis pigmentosa. Recently, OFD1 pathogenic variants have been implicated in primary ciliary dyskinesia (PCD), a disorder of the motile cilia with a phenotype that includes recurrent oto‐sino‐pulmonary infections, situs abnormalities, and decreased fertility. Methods We describe three male patients with PCD who were found to have hemizygous pathogenic variants in OFD1, further supporting that PCD is part of a clinical spectrum of OFD1‐related disorders. In addition, we provide a review of the available clinical literature describing patients with OFD1 variants and highlight the phenotypic variability of OFD1‐related disease. Results Some individuals with hemizygous OFD1 variants have PCD, either apparently isolated or in combination with other features of OFD1‐related disorders. Conclusion As clinicians consider the presence or absence of conditions allelic at OFD1, PCD should be considered part of the spectrum of OFD1‐related disorders. Understanding the OFD1‐related disease spectrum may allow for more focused genetic testing and more timely management of treatable sequelae.

Published

2019

4. Recurring large deletion in DRC1 (CCDC164) identified as causing primary ciliary dyskinesia in two Asian patients

Author

Kozo Morimoto, Minako Hijikata, Maimoona A. Zariwala, Keith Nykamp, Atsushi Inaba, Tz‐Chun Guo, Hiroyuki Yamada, Rebecca Truty, Yuka Sasaki, Ken Ohta, Shoji Kudoh, Margaret W. Leigh, Michael R. Knowles, and Naoto Keicho

Subjects

Asia, diffuse panbronchiolitis, DRC1, primary ciliary dyskinesia, recurrent mutation, Genetics, QH426-470

Abstract

Abstract Background Primary ciliary dyskinesia (PCD) is a relatively rare autosomal recessive or X‐linked disorder affecting ciliary function. In the set of causative genes, however, predominant pathogenic variants remain unknown in Asia. Method A diagnosis of PCD was made following a modern comprehensive testing including genetic analysis; targeted resequencing for screening variants, and Sanger sequencing for determination of the breakpoints, with an additional review of databases to calculate the deletion frequency. A multiplexed PCR‐based detection method has also been developed. Results We ascertained a 50‐year‐old Japanese male who had been diagnosed with diffuse panbronchiolitis (DPB), but refractory to macrolide therapy. We reevaluated the case and identified a large homozygous deletion spanning exons 1 to 4 of the DRC1 and determined the breakpoints (NM_145038.4: c.1‐3952_540 + 1331del27748‐bp). In the PCD cohort at the University of North Carolina, we found a female PCD patient of Korean descent harboring the same homozygous deletion. From the Invitae testing cohort, we extracted four carriers of the same deletion among 965 Asian individuals, whereas no deletion was found in the 23,951 non‐Asians. Conclusion We speculate that the DRC1 deletion is a recurrent or perhaps founder mutation in Asians. The simple PCR method could be a useful screening tool.

Published

2019

5. Airway Disease in Children with Primary Ciliary Dyskinesia: Impact of Ciliary Ultrastructure Defect and Genotype

Author

BreAnna Kinghorn, Margaret Rosenfeld, Erin Sullivan, Frankline Onchiri, Thomas W. Ferkol, Scott D. Sagel, Sharon D. Dell, Carlos Milla, Adam J. Shapiro, Kelli M. Sullivan, Maimoona A. Zariwala, Jessica E. Pittman, Federico Mollica, Harm A. W. M. Tiddens, Mariette Kemner-van de Corput, Michael R. Knowles, Stephanie D. Davis, and Margaret W. Leigh

Subjects

Pulmonary and Respiratory Medicine

Abstract

Primary ciliary dyskinesia (PCD) is characterized by impaired mucociliary clearance, recurrent respiratory infections, and progressive airway damage and obstructive lung disease. While the association of ciliary ultrastructure defect/genotype with severity of airflow obstruction has been well characterized, their association with airway abnormalities on chest computed tomography (CT) has been minimally evaluated.We sought to delineate the association of ciliary defect class/genotype with chest CT scores in children with PCD.Cross-sectional analysis of children with PCD (N=146) enrolled in a prospective multicenter observational study, stratified by defect type: ODA (outer dynein arm), ODA/IDA (outer and inner dynein arm), IDA/MTD (inner dynein arm and microtubular disorganization), and Normal/Near Normal ultrastructure with associated genotypes. CTs were scored utilizing the Melbourne-Rotterdam Annotated Grid Morphometric Analysis for PCD (MERAGMA-PCD), evaluating airway abnormalities in a hierarchical order: atelectasis, bronchiectasis, bronchial wall thickening, mucus plugging/tree in bud opacities. Volume fraction of each component was expressed as % of total lung volume. %Disease was computed as the sum of all components. Regression analyses were utilized to describe the association between clinical predictors and CT scores.Acceptable chest CTs were obtained in 141 children (71 male): 57 ODA, 20 ODA/IDA, 40 IDA/MTD, 24 Normal/Near Normal. Mean (SD) age was 8.5 (4.6) years, forced expiratory volume in 1 second (FEV1) % predicted was 82.4 (19.5), and %Disease was 4.6 (3.5). Children with IDA/MTD defects had higher %Disease compared to children with ODA defects (2.71% higher (95%CI: 1.37-4.06, p0.001)), driven by higher %Mucus plugging (2.35% higher (1.43-3.26, p0.001)). Increasing age, lower BMI, and lower FEV1 were associated with higher %Disease (0.23%, 95%CI: 0.11-0.35, p0.001; 0.03%, 95%CI: 0.01-0.04, p=0.008; and 0.05%, 95%CI: 0.01-0.08, p=0.011, respectively).Children with IDA/MTD defects had significantly greater airway disease on CT, primarily mucus plugging, compared to children with ODA defects.

Published

2023

6. Association of Neonatal Hospital Length of Stay with Lung Function in Primary Ciliary Dyskinesia

Author

Wallace B. Wee, Margaret W. Leigh, Stephanie D. Davis, Margaret Rosenfeld, Kelli M. Sullivan, Michael G. Sawras, Thomas W. Ferkol, Michael R. Knowles, Carlos Milla, Scott D. Sagel, Maimoona A. Zariwala, Eleanor Pullenayegum, and Sharon D. Dell

Subjects

Pulmonary and Respiratory Medicine, Male, Adolescent, Kartagener Syndrome, Infant, Newborn, Infant, Length of Stay, Hospitals, Cohort Studies, Child, Preschool, Humans, Prospective Studies, Child, Lung, Ciliary Motility Disorders

Published

2023

7. A Deep Intronic, Pathogenic Variant in

Author

Adam J, Shapiro, Jaclyn R, Stonebraker, Michael R, Knowles, and Maimoona A, Zariwala

Subjects

Kartagener Syndrome, Mutation, Humans, Axonemal Dyneins, Cilia

Published

2023

8. Laterality Defects in Primary Ciliary Dyskinesia: Relationship to Ultrastructural Defect or Genotype

Author

Andrew T. Barber, Adam J. Shapiro, Stephanie D. Davis, Thomas W. Ferkol, Jeffrey J. Atkinson, Scott D. Sagel, Sharon D. Dell, Kenneth N. Olivier, Carlos E. Milla, Margaret Rosenfeld, Lang Li, Feng-Chang Lin, Kelli M. Sullivan, Nicole A. Capps, Maimoona A. Zariwala, Michael R. Knowles, and Margaret W. Leigh

Subjects

Pulmonary and Respiratory Medicine

Abstract

The association between organ laterality abnormalities and ciliary ultrastructural defect or genotype in primary ciliary dyskinesia is poorly understood.To determine if there is an association between presence/type of laterality abnormality and ciliary ultrastructural defect and genotype.Participants with primary ciliary dyskinesia in a multicenter, prospective study were grouped based on ciliary ultrastructural defect or genotype. In a retrospective analysis of this data, the association of ciliary ultrastructural defect or genotype and likelihood of a laterality abnormality was evaluated by logistic regression adjusted for presence of two loss-of-function versus one or more not-loss-of-function variants.Of 559 participants, 286 (51.2%), 215 (38.5%), and 58 (10.4%) were identified as having situs solitus, situs inversus totalis, and situs ambiguus, respectively; heterotaxy, defined as situs ambiguus with complex cardiovascular defects, was present in 14 (2.5%). Compared to group with inner dynein arm defects with microtubular disorganization, laterality defects were more likely in the outer dynein arm defects group (OR 2.07, 95% CI 1.21-3.54, P0.01) and less likely in the normal/near normal ultrastructure group (OR 0.04, 95% CI 0.013-0.151, P0.01). Heterotaxy was present in 11 of 242 (4.5%) in the outer dynein arm defects group but zero of 96 in the inner dynein arm defects with microtubular disorganization group (P=0.038).In primary ciliary dyskinesia, risk of a laterality abnormality differs by ciliary ultrastructure defect. Pathophysiologic mechanisms underlying these differences require further exploration.

Published

2023

9. HYDINVariants Are a Common Cause of Primary Ciliary Dyskinesia in French Canadians

Author

Adam J. Shapiro, Guillaume Sillon, Daniela D’Agostino, Laurence Baret, Francesc López-Giráldez, Shrikant Mane, Margaret W. Leigh, Stephanie D. Davis, Michael R. Knowles, and Maimoona A. Zariwala

Subjects

Pulmonary and Respiratory Medicine

Published

2023

10. A Deep Intronic, Pathogenic Variant in DNAH11 Causes Primary Ciliary Dyskinesia

Author

Adam J. Shapiro, Jaclyn R. Stonebraker, Michael R. Knowles, and Maimoona A. Zariwala

Subjects

Pulmonary and Respiratory Medicine, Clinical Biochemistry, Cell Biology, Molecular Biology

Published

2022

11. First reports of primary ciliary dyskinesia caused by a shared DNAH11 allele in Canadian Inuit

Author

Julia Hunter‐Schouela, Michael T. Geraghty, Robert A. Hegele, David A. Dyment, David St Pierre, Julie Richer, Holden Sheffield, Maimoona A. Zariwala, Michael R. Knowles, Anna Lehman, Sharon Dell, Adam J. Shapiro, and Thomas A. Kovesi

Subjects

Pulmonary and Respiratory Medicine, Pediatrics, Perinatology and Child Health

Published

2023

12. Hereditary Mucin Deficiency Caused by Biallelic Loss of Function of MUC5B

Author

Gregory Costain, Zhen Liu, Vito Mennella, Giorgia Radicioni, Adrienn N. Goczi, Alexandra Albulescu, Susan Walker, Bo Ngan, David Manson, Reza Vali, Meraj Khan, Nades Palaniyar, David B. Hill, David A. Hall, Christian R. Marshall, Michael Knowles, Maimoona A. Zariwala, Mehmet Kesimer, and Sharon D. Dell

Subjects

Pulmonary and Respiratory Medicine, Critical Care and Intensive Care Medicine

Published

2022

13. Going beyond the chest X‐ray: Investigating laterality defects in primary ciliary dyskinesia

Author

Wallace B. Wee, Kimberley R. Kaspy, Michael G. Sawras, Michael R. Knowles, Maimoona A. Zariwala, Margaret W. Leigh, Sharon D. Dell, and Adam J. Shapiro

Subjects

Adult, Pulmonary and Respiratory Medicine, Canada, Kartagener Syndrome, X-Rays, Respiration Disorders, Situs Inversus, Article, Radiography, Pediatrics, Perinatology and Child Health, otorhinolaryngologic diseases, Humans, Child, Ciliary Motility Disorders, Retrospective Studies

Abstract

BACKGROUND: Organ laterality defects in primary ciliary dyskinesia (PCD) are common, ranging from complete mirror image organ arrangement, situs inversus totalis (SIT), to situs ambiguus (SA), which falls along the spectrum of situs solitus (SS) and SIT. Targeted investigations for organ laterality defects are not universally recommended in PCD consensus statements. Without investigations beyond chest radiography (CXR), clinically significant defects may go undetected leading to increased morbidity. We hypothesize that clinically significant SA defects remain undetected on CXR and targeted investigations are needed to detect various laterality defects associated with morbidity. METHODS: This retrospective study collected data from PCD clinics at two Canadian children’s hospitals from 2012 to 2020. Participants

Published

2022

14. Otolaryngology Manifestations of Primary Ciliary Dyskinesia: A Multicenter Study

Author

Sharon D. Dell, Faisal Zawawi, Nikolaus E. Wolter, Adam J. Shapiro, Maimoona A. Zariwala, Mariana M. Smith, Michael R. Knowles, Pilar Gajardo, Cinzia L. Marchica, Margaret W. Leigh, and Sam J. Daniel

Subjects

Pediatrics, medicine.medical_specialty, business.industry, medicine.disease, Article, Otolaryngology, 03 medical and health sciences, Cross-Sectional Studies, 0302 clinical medicine, 030228 respiratory system, Otorhinolaryngology, Multicenter study, Quality of life, Quality of Life, otorhinolaryngologic diseases, medicine, Humans, Surgery, Sinusitis, Child, 030223 otorhinolaryngology, business, Ciliary Motility Disorders, Primary ciliary dyskinesia

Abstract

OBJECTIVE. This project aims to prospectively and objectively assess otolaryngological manifestations and quality of life of children with primary ciliary dyskinesia (PCD) and compare these findings with healthy pediatric controls. STUDY DESIGN. Cross-sectional. SETTING. Two high-volume pediatric PCD specialty centers. METHODS. Standardized clinical assessment; Sino-Nasal Outcome Test 22 (SNOT-22); Hearing Environment and Reflection Quality of Life (HEAR-QL); Reflux Symptom Index (RSI); standardized physical examination of the sinonasal, laryngeal, and otological systems; and investigations including pure-tone audiograms (PTAs) and sinonasal cultures were collected. RESULTS. Forty-seven children with PCD and 25 control participants were recruited. Children with PCD had more upper airway symptoms than healthy children. They had significantly higher scores in both SNOT-22 and RSI, indicating worse sinonasal and reflux symptoms, with worse quality of life on the HEAR-QL index compared to healthy children (P < .05). Fifty-two percent of children with PCD-related hearing loss were not aware of their hearing deficit that was present on audiological assessment, and only 23% of children who had ventilation tubes had chronic otorrhea, most of which was easily controlled with ototopic drops. Furthermore, although all children with PCD had chronic rhinosinusitis, only 36% of them were using topical nasal treatment. The most common bacteria cultured from the middle meatus were Staphylococcus aureus in 11 of 47 (23%), followed by Streptococcus pneumoniae in 10 of 47 (21%). CONCLUSION. This multisite cohort highlights the importance of otolaryngology involvement in the management of children with PCD. More rigorous otolaryngological management may lead to reductions in overall morbidity and improve quality of life for children with PCD.

Published

2021

15. Structural insights into the cause of human RSPH4A primary ciliary dyskinesia

Author

Jianfeng Lin, Michael R. Knowles, L.A. Daniels, Lawrence E. Ostrowski, Patrick R. Sears, Yanhe Zhao, Maimoona A. Zariwala, Justine M Pinskey, Weining Yin, and Daniela Nicastro

Subjects

0303 health sciences, 03 medical and health sciences, 0302 clinical medicine, medicine, Cell Biology, Biology, Bioinformatics, medicine.disease, Molecular Biology, 030217 neurology & neurosurgery, 030304 developmental biology, Primary ciliary dyskinesia

Abstract

A growing number of ciliopathy-associated genes have been identified, but how they cause ciliary dysfunction is often unclear. Using cryo-electron tomography, we characterize the structural defects in patient cilia lacking radial spoke protein RSPH4A, revealing the underlying molecular defects and providing new insight into ciliary disease etiology.

Published

2021

16. Use caution interpreting nasal nitric oxide: Overlap in primary ciliary dyskinesia and primary immunodeficiency

Author

Hannah Boutros, Stephanie D. Davis, Maimoona A. Zariwala, Michael R. Knowles, Margaret W. Leigh, and Andrew T. Barber

Subjects

Pulmonary and Respiratory Medicine, medicine.medical_specialty, Kartagener Syndrome, business.industry, Nose, Nitric Oxide, medicine.disease, Dermatology, Article, Nitric oxide, chemistry.chemical_compound, chemistry, Pediatrics, Perinatology and Child Health, Primary immunodeficiency, Humans, Medicine, Use caution, business, Ciliary Motility Disorders, Primary ciliary dyskinesia

Published

2021

17. A human ciliopathy reveals essential functions for NEK10 in airway mucociliary clearance

Author

Patrick R. Sears, Hanan E. Shamseldin, Heymut Omran, Katharine E. Black, Maimoona A. Zariwala, Vladimir Vinarsky, Evgeni M. Frenkel, David M. Sabatini, Hui Min Leung, Fowzan S. Alkuraya, Michael R. Knowles, Guillermo J. Tearney, Lida P. Hariri, M. Leigh Anne Daniels, Jason H. Yang, Martin S. Taylor, Raghu R. Chivukula, Johnny L. Carson, Ibrahim Almogarri, Daniel T. Montoro, and Gerard W. Dougherty

Subjects

0301 basic medicine, Cell type, biology, Mucociliary clearance, General Medicine, medicine.disease, Cystic fibrosis, Article, General Biochemistry, Genetics and Molecular Biology, Cystic fibrosis transmembrane conductance regulator, Cell biology, 03 medical and health sciences, Ciliopathy, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, medicine, biology.protein, Motile cilium, Stem cell, Primary ciliary dyskinesia

Abstract

Mucociliary clearance, the physiological process by which mammalian conducting airways expel pathogens and unwanted surface materials from the respiratory tract, depends on the coordinated function of multiple specialized cell types, including basal stem cells, mucus-secreting goblet cells, motile ciliated cells, cystic fibrosis transmembrane conductance regulator (CFTR)-rich ionocytes, and immune cells1,2. Bronchiectasis, a syndrome of pathological airway dilation associated with impaired mucociliary clearance, may occur sporadically or as a consequence of Mendelian inheritance, for example in cystic fibrosis, primary ciliary dyskinesia (PCD), and select immunodeficiencies3. Previous studies have identified mutations that affect ciliary structure and nucleation in PCD4, but the regulation of mucociliary transport remains incompletely understood, and therapeutic targets for its modulation are lacking. Here we identify a bronchiectasis syndrome caused by mutations that inactivate NIMA-related kinase 10 (NEK10), a protein kinase with previously unknown in vivo functions in mammals. Genetically modified primary human airway cultures establish NEK10 as a ciliated-cell-specific kinase whose activity regulates the motile ciliary proteome to promote ciliary length and mucociliary transport but which is dispensable for normal ciliary number, radial structure, and beat frequency. Together, these data identify a novel and likely targetable signaling axis that controls motile ciliary function in humans and has potential implications for other respiratory disorders that are characterized by impaired mucociliary clearance. Inactivating mutations in a protein kinase, NEK10, cause a genetic bronchiectasis syndrome in humans that is characterized by short motile cilia and impaired mucociliary transport.

Published

2020

18. The role of SPAG1 in the assembly of axonemal dyneins in human airway epithelia

Author

Amanda J. Smith, Ximena M. Bustamante-Marin, Weining Yin, Patrick R. Sears, Laura E. Herring, Nedyalka N. Dicheva, Francesc López-Giráldez, Shrikant Mane, Robert Tarran, Margaret W. Leigh, Michael R. Knowles, Maimoona A. Zariwala, and Lawrence E. Ostrowski

Subjects

Axoneme, GTP-Binding Proteins, Antigens, Surface, Mutation, Respiratory System, Dyneins, Humans, macromolecular substances, Cell Biology, Axonemal Dyneins, Cilia, Research Article

Abstract

Mutations in SPAG1, a dynein axonemal assembly factor (DNAAF) that facilitates the assembly of dynein arms in the cytoplasm before their transport into the cilium, result in primary ciliary dyskinesia (PCD), a genetically heterogenous disorder characterized by chronic oto-sino-pulmonary disease, infertility and laterality defects. To further elucidate the role of SPAG1 in dynein assembly, we examined its expression, interactions and ciliary defects in control and PCD human airway epithelia. Immunoprecipitations showed that SPAG1 interacts with multiple DNAAFs, dynein chains and canonical components of the R2TP complex. Protein levels of dynein heavy chains (DHCs) and interactions between DHCs and dynein intermediate chains (DICs) were reduced in SPAG1 mutants. We also identified a previously uncharacterized 60 kDa SPAG1 isoform, through examination of PCD subjects with an atypical ultrastructural defect for SPAG1 variants, that can partially compensate for the absence of full-length SPAG1 to assemble a reduced number of outer dynein arms. In summary, our data show that SPAG1 is necessary for axonemal dynein arm assembly by scaffolding R2TP-like complexes composed of several DNAAFs that facilitate the folding and/or binding of the DHCs to the DIC complex.

Published

2022

19. Expression of a Truncated Form of

Author

Lawrence E, Ostrowski, Weining, Yin, Amanda J, Smith, Patrick R, Sears, Ximena M, Bustamante-Marin, Hong, Dang, Friedhelm, Hildebrandt, Leigh Anne, Daniels, Nicole A, Capps, Kelli M, Sullivan, Margaret W, Leigh, Maimoona A, Zariwala, and Michael R, Knowles

Subjects

Adult, Male, Adolescent, Dyneins, Middle Aged, Phenotype, Case-Control Studies, Mutation, Humans, Female, Mutant Proteins, Cilia, RNA, Messenger, Child, Microtubule-Associated Proteins, Ciliary Motility Disorders

Abstract

Primary ciliary dyskinesia (PCD) is a rare lung disease caused by mutations that impair the function of motile cilia, resulting in chronic upper and lower respiratory disease, reduced fertility, and a high prevalence of situs abnormalities. The disease is genetically and phenotypically heterogeneous, with causative mutations in50 genes identified, and clinical phenotypes ranging from mild to severe. Absence of

Published

2021

20. Identification of genetic variants in CFAP221 as a cause of primary ciliary dyskinesia

Author

Maimoona A. Zariwala, Wu Lin Charng, Michael R. Knowles, Patrick R. Sears, Adam J. Shapiro, Lawrence E. Ostrowski, Donald F. Conrad, Margaret W. Leigh, and Ximena M. Bustamante-Marin

Subjects

0301 basic medicine, Candidate gene, CFAP221, 030105 genetics & heredity, Biology, Compound heterozygosity, Article, 03 medical and health sciences, Primary ciliary dyskinesia, Exome Sequencing, Genetic variation, otorhinolaryngologic diseases, Genetics, medicine, Humans, ciliary waveform, Cilia, Allele, PCDP1, Alleles, Genetics (clinical), Exome sequencing, Cilium, Genetic Variation, Proteins, Epithelial Cells, Exons, PCD, medicine.disease, 030104 developmental biology, Mutation, Motile cilium, Calmodulin-Binding Proteins, Ciliary Motility Disorders

Abstract

Primary ciliary dyskinesia (PCD) is a rare disorder that affects the biogenesis or function of motile cilia resulting in chronic airway disease. PCD is genetically and phenotypically heterogeneous, with causative mutations identified in over 40 genes; however, the genetic basis of many cases is unknown. Using whole-exome sequencing, we identified three affected siblings with clinical symptoms of PCD but normal ciliary structure, carrying compound heterozygous loss-of-function variants in CFAP221. Computational analysis suggests that these variants are the most damaging alleles shared by all three siblings. Nasal epithelial cells from one of the subjects demonstrated slightly reduced beat frequency (16.5 Hz vs 17.7 Hz, p = 0.16); however, waveform analysis revealed that the CFAP221 defective cilia beat in an aberrant circular pattern. These results show that genetic variants in CFAP221 cause PCD and that CFAP221 should be considered a candidate gene in cases where PCD is suspected but cilia structure and beat frequency appear normal.

Published

2019

21. Primary ciliary dyskinesia (PCD): A genetic disorder of motile cilia

Author

Maimoona A. Zariwala, Margaret W. Leigh, BreAnna Kinghorn, Amjad Horani, Michael R. Knowles, and Michael Glenn O’Connor

Subjects

Pathology, medicine.medical_specialty, Motile cilium, medicine, Genetic disorder, General Medicine, Biology, medicine.disease, Article, Primary ciliary dyskinesia

Published

2019

22. Lack of GAS2L2 Causes PCD by Impairing Cilia Orientation and Mucociliary Clearance

Author

Michael E. Werner, Troy D. Rogers, Eva J. Brotslaw, Barbara R. Grubb, Maimoona A. Zariwala, Brian J. Mitchell, Michael R. Knowles, Corey M. Jania, Serge Amselem, Marie Legendre, Estelle Escudier, Ximena M. Bustamante-Marin, Patrick R. Sears, Lucie Thomas, L. Réfabert, Wei Ning Yin, Kirby L. Zeman, Laura E. Herring, Lawrence E. Ostrowski, University of North Carolina [Chapel Hill] (UNC), University of North Carolina System (UNC), Northwestern University [Chicago, Ill. USA], Service de Pneumologie Allergologie [CHU Necker], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-CHU Necker - Enfants Malades [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Université Paris Descartes - Paris 5 (UPD5), Maladies génétiques d'expression pédiatrique [CHU Trousseau] (Inserm U933), Institut National de la Santé et de la Recherche Médicale (INSERM)-CHU Trousseau [APHP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), UF de Génétique moléculaire [CHU Trousseau], CHU Trousseau [APHP], and Couvet, Sandrine

Subjects

Male, 0301 basic medicine, Rotation, Morpholino, Mucociliary clearance, Xenopus, primary ciliary dyskinesia, Xenopus Proteins, [SDV.GEN.GH] Life Sciences [q-bio]/Genetics/Human genetics, Biology, Compound heterozygosity, Article, Frameshift mutation, Mice, 03 medical and health sciences, Exon, 0302 clinical medicine, Genetics, medicine, Animals, Humans, mucociliary clearance, Basal body, Cilia, Genetics (clinical), Primary ciliary dyskinesia, Mice, Knockout, MCC, Cilium, Microfilament Proteins, Exons, PCD, medicine.disease, Molecular biology, Disease Models, Animal, GAS2L2, Phenotype, 030104 developmental biology, [SDV.GEN.GH]Life Sciences [q-bio]/Genetics/Human genetics, Female, Genes, Lethal, Microtubule-Associated Proteins, Gene Deletion, 030217 neurology & neurosurgery, Ciliary Motility Disorders, ciliary orientation

Abstract

International audience; Primary ciliary dyskinesia (PCD) is a genetic disorder in which impaired ciliary function leads to chronic airway disease. Exome sequencing of a PCD subject identified an apparent homozygous frameshift variant, c.887_890delTAAG (p.Val296Glyfs∗13), in exon 5; this frameshift introduces a stop codon in amino acid 308 of the growth arrest-specific protein 2-like 2 (GAS2L2). Further genetic screening of unrelated PCD subjects identified a second proband with a compound heterozygous variant carrying the identical frameshift variant and a large deletion (c.867_∗343+1207del; p.?) starting in exon 5. Both individuals had clinical features of PCD but normal ciliary axoneme structure. In this research, using human nasal cells, mouse models, and X.laevis embryos, we show that GAS2L2 is abundant at the apical surface of ciliated cells, where it localizes with basal bodies, basal feet, rootlets, and actin filaments. Cultured GAS2L2-deficient nasal epithelial cells from one of the affected individuals showed defects in ciliary orientation and had an asynchronous and hyperkinetic (GAS2L2-deficient = 19.8 Hz versus control = 15.8 Hz) ciliary-beat pattern. These results were recapitulated in Gas2l2-/- mouse tracheal epithelial cell (mTEC) cultures and in X. laevis embryos treated with Gas2l2 morpholinos. In mice, the absence of Gas2l2 caused neonatal death, and the conditional deletion of Gas2l2 impaired mucociliary clearance (MCC) and led to mucus accumulation. These results show that a pathogenic variant in GAS2L2 causes a genetic defect in ciliary orientation and impairs MCC and results in PCD

Published

2019

23. Autosomal dominant variants in FOXJ1 causing primary ciliary dyskinesia in two patients with obstructive hydrocephalus

Author

Lyne Joyal, Michael R. Knowles, M Leigh Ann Daniels, Jaclyn R. Stonebraker, Van-Hung Nguyen, Maimoona A. Zariwala, Kimberley Kaspy, and Adam J. Shapiro

Subjects

Male, 0301 basic medicine, Proband, Pathology, medicine.medical_specialty, Mucociliary clearance, QH426-470, 030105 genetics & heredity, 03 medical and health sciences, Genetics, medicine, Humans, Molecular Biology, Genetics (clinical), Genes, Dominant, Primary ciliary dyskinesia, Bronchiectasis, business.industry, Cilium, Infant, Forkhead Transcription Factors, Original Articles, Middle Aged, medicine.disease, Hydrocephalus, Situs inversus, Phenotype, 030104 developmental biology, Mutation, Motile cilium, Original Article, Female, business, Ciliary Motility Disorders

Abstract

Background Primary ciliary dyskinesia (PCD) is a mostly autosomal recessive, genetic disease of abnormal motile cilia function, resulting in bronchiectasis, infertility, organ laterality defects, and chronic otolaryngology disease. Though motile, ependymal cilia influencing cerebrospinal fluid flow in the central nervous system share many aspects of structure and function with motile cilia in the respiratory tract, hydrocephalus is rarely associated with PCD. Recently, pathogenic variants in FOXJ1 (Chr 17q25.1) were identified causing PCD associated with hydrocephalus, reduced respiratory cilia number, axonemal microtubule disorganization, and occurring in a de novo, autosomal dominant inheritance pattern. Method Two patients with chronic oto‐sino‐pulmonary disease and hydrocephalus underwent candidate testing of FOXJ1. Coding region and splice junctions were sequenced and analyzed under the auspices of Genetic Disorders of Mucociliary Clearance Consortium. Results Upon sequencing of the entire coding region and splice‐junctions, heterozygous, pathogenic variants in FOXJ1 were discovered in exon 3 of two patients: an 11‐month‐old female with situs inversus totalis (NM_001454.4: c.945delC (p.Phe315Leufs*18)) and a 51 year‐old male, post‐double lung transplantation (NM_001454.4: c.929_932delACTG (p.Asp310Glyfs*22)). FOXJ1 variants were not detected in the available parents and the siblings of these probands. Conclusion FOXJ1 pathogenic variants cause PCD in a de novo, autosomal dominant inheritance pattern, and are associated with hydrocephalus. Physicians treating patients with hydrocephalus and chronic oto‐sino‐pulmonary disease should be aware of this PCD association and test for FOXJ1 variants., Variants in FOXJ1 are a rare cause of respiratory ciliary dysfunction and hydrocephalus, but few cases have been previously illustrated. We report 2 cases of primary ciliary dyskinesia (PCD) with hydrocephalus, both caused by de novo, autosomal dominant, variants in FOXJ1. FOXJ1 should be examined in patients with hydrocephalus and classic PCD symptoms of chronic oto‐sino‐pulmonary disease, neonatal respiratory distress, and organ laterality defects.

Published

2021

24. Structural insights into the cause of human

Author

Yanhe, Zhao, Justine, Pinskey, Jianfeng, Lin, Weining, Yin, Patrick R, Sears, Leigh A, Daniels, Maimoona A, Zariwala, Michael R, Knowles, Lawrence E, Ostrowski, and Daniela, Nicastro

Subjects

Cytoskeletal Proteins, Electron Microscope Tomography, Axoneme, Mutation, Respiratory System, Humans, Cilia, Articles, Ciliary Motility Disorders

Abstract

Cilia and flagella are evolutionarily conserved eukaryotic organelles involved in cell motility and signaling. In humans, mutations in Radial Spoke Head Component 4A (RSPH4A) can lead to primary ciliary dyskinesia (PCD), a life-shortening disease characterized by chronic respiratory tract infections, abnormal organ positioning, and infertility. Despite its importance for human health, the location of RSPH4A in human cilia has not been resolved, and the structural basis of RSPH4A–/– PCD remains elusive. Here, we present the native three-dimensional structure of RSPH4A–/– human respiratory cilia using samples collected noninvasively from a PCD patient. Using cryo–electron tomography (cryo-ET) and subtomogram averaging, we compared the structures of control and RSPH4A–/– cilia, revealing primary defects in two of the three radial spokes (RSs) within the axonemal repeat and secondary (heterogeneous) defects in the central pair complex. Similar to RSPH1–/– cilia, the radial spoke heads of RS1 and RS2, but not RS3, were missing in RSPH4A–/– cilia. However, RSPH4A–/– cilia also exhibited defects within the arch domains adjacent to the RS1 and RS2 heads, which were not observed with RSPH1 loss. Our results provide insight into the underlying structural basis for RSPH4A–/– PCD and highlight the benefits of applying cryo-ET directly to patient samples for molecular structure determination.

Published

2021

25. Motile ciliopathies

Author

Julia Wallmeier, Kim G. Nielsen, Claudia E. Kuehni, Jane S. Lucas, Margaret W. Leigh, Maimoona A. Zariwala, and Heymut Omran

Subjects

otorhinolaryngologic diseases, General Medicine

Abstract

Motile cilia are highly complex hair-like organelles of epithelial cells lining the surface of various organ systems. Genetic mutations (usually with autosomal recessive inheritance) that impair ciliary beating cause a variety of motile ciliopathies, a heterogeneous group of rare disorders. The pathogenetic mechanisms, clinical symptoms and severity of the disease depend on the specific affected genes and the tissues in which they are expressed. Defects in the ependymal cilia can result in hydrocephalus, defects in the cilia in the fallopian tubes or in sperm flagella can cause female and male subfertility, respectively, and Malfunctional motile monocilia of the left–right organizer during early embryonic development can lead to laterality defects such as situs inversus and heterotaxy. If muco-ciliary clearance in the respiratory epithelium is severely impaired, the disorder is referred to as primary ciliary dyskinesia (PCD), the most common motile ciliopathy. No single test can confirm a diagnosis of motile ciliopathy, which is based on a combination of tests including nasal nitric oxide measurement; TEM, immunofluorescence and genetic analyses; and high-speed video microscopy. With the exception of azithromycin, there is no evidence-based treatment for PCD; therapies aim at relieving symptoms and reduce the effects of reduced ciliary motility.

Published

2020

26. Mutation of CFAP57, a protein required for the asymmetric targeting of a subset of inner dynein arms in Chlamydomonas, causes primary ciliary dyskinesia

Author

Mathieu Bottier, Hailey Bowen, Amjad Horani, Lawrence E. Ostrowski, Maimoona A. Zariwala, Wei Ning Yin, L.A. Daniels, Donald F. Conrad, Wu Lin Charng, Michael R. Knowles, Ximena M. Bustamante-Marin, Susan K. Dutcher, Mihaela Stoyanova, and Patrick R. Sears

Subjects

Axoneme, Male, Cancer Research, Heredity, Physiology, QH426-470, Pathology and Laboratory Medicine, Biochemistry, Homozygosity, Epithelium, Mice, 0302 clinical medicine, Animal Cells, Medicine and Health Sciences, Genetics (clinical), Cells, Cultured, Conserved Sequence, Primary ciliary dyskinesia, Plant Proteins, 0303 health sciences, Cilium, Microtubule Motors, 3T3 Cells, Cell biology, Codon, Nonsense, Motile cilium, Cellular Structures and Organelles, Pathogens, Cellular Types, Anatomy, Microtubule-Associated Proteins, Research Article, Ciliary Motility Disorders, Pathogen Motility, Adult, Virulence Factors, Dynein, Motor Proteins, Respiratory Mucosa, Biology, 03 medical and health sciences, Autosomal recessive trait, Intraflagellar transport, Molecular Motors, medicine, Genetics, Animals, Humans, Cilia, Molecular Biology, Ecology, Evolution, Behavior and Systematics, Swimming, 030304 developmental biology, Biological Locomotion, Biology and Life Sciences, Proteins, Dyneins, Human Genetics, Epithelial Cells, Cell Biology, medicine.disease, Cytoskeletal Proteins, Biological Tissue, Inner dynein arm assembly, 030217 neurology & neurosurgery, Chlamydomonas reinhardtii

Abstract

Primary ciliary dyskinesia (PCD) is characterized by chronic airway disease, reduced fertility, and randomization of the left/right body axis. It is caused by defects of motile cilia and sperm flagella. We screened a cohort of affected individuals that lack an obvious axonemal defect for pathogenic variants using whole exome capture, next generation sequencing, and bioinformatic analysis assuming an autosomal recessive trait. We identified one subject with an apparently homozygous nonsense variant [(c.1762C>T), p.(Arg588*)] in the uncharacterized CFAP57 gene. Interestingly, the variant results in the skipping of exon 11 (58 amino acids), which may be due to disruption of an exonic splicing enhancer. In normal human nasal epithelial cells, CFAP57 localizes throughout the ciliary axoneme. Nasal cells from the PCD patient express a shorter, mutant version of CFAP57 and the protein is not incorporated into the axoneme. The missing 58 amino acids include portions of WD repeats that may be important for loading onto the intraflagellar transport (IFT) complexes for transport or docking onto the axoneme. A reduced beat frequency and an alteration in ciliary waveform was observed. Knockdown of CFAP57 in human tracheobronchial epithelial cells (hTECs) recapitulates these findings. Phylogenetic analysis showed that CFAP57 is highly conserved in organisms that assemble motile cilia. CFAP57 is allelic with the BOP2/IDA8/FAP57 gene identified previously in Chlamydomonas reinhardtii. Two independent, insertional fap57 Chlamydomonas mutant strains show reduced swimming velocity and altered waveforms. Tandem mass tag (TMT) mass spectroscopy shows that FAP57 is missing, and the “g” inner dyneins (DHC7 and DHC3) and the “d” inner dynein (DHC2) are reduced, but the FAP57 paralog FBB7 is increased. Together, our data identify a homozygous variant in CFAP57 that causes PCD that is likely due to a defect in the inner dynein arm assembly process., Author summary Primary ciliary dyskinesia (PCD) is a rare genetic disease that affects the function of motile cilia. The estimated incidence is about 1 in 15,000 births, but diagnosis can be difficult since it is genetically heterogenous. At present, about 30% of PCD patients lack a genetic diagnosis. By applying whole exome sequencing and bioinformatic analysis, we identified a variant in an uncharacterized gene, CFAP57, in a subject previously diagnosed with PCD. This is the first reported example of PCD caused by a mutation that likely only affects a subset of the inner dynein arms. These findings demonstrate the effectiveness of whole exome sequencing and bioinformatic analysis for identifying pathogenic variants in rare genetic diseases like PCD, expand our understanding of how dynein arms are positioned during cilia assembly, and identify a variant in CFAP57 that causes PCD.

Published

2020

27. Association of Genotype and Structural Lung Disease in a Cohort of Children with PCD

Author

Erin Sullivan, Carlos Milla, M. Kemner-van de Corput, Jessica E. Pittman, BreAnna Kinghorn, Michael R. Knowles, Frankline Onchiri, Sharon D. Dell, Margaret W. Leigh, Adam J. Shapiro, Maimoona A. Zariwala, Margaret Rosenfeld, Thomas W. Ferkol, Kelli M. Sullivan, Harm A.W.M. Tiddens, F. Mollica, Stephanie D. Davis, and Scott D. Sagel

Subjects

Oncology, medicine.medical_specialty, Lung disease, business.industry, Association (object-oriented programming), Internal medicine, Cohort, Genotype, medicine, business

Published

2020

28. Hereditary Mucin Deficiency Caused by Biallelic Loss-of-Function of MUC5B Defines a Novel Category of Lung Disease

Author

Mehmet Kesimer, Maimoona A. Zariwala, Zhen Liu, G. Costain, A. Goczi, Michael R. Knowles, David A. Hall, Sharon D. Dell, S. Walker, Christian R. Marshall, B. Ngan, Vito Mennella, and Alexandra Albulescu

Subjects

Pathology, medicine.medical_specialty, Lung disease, business.industry, Mucin, medicine, business, Loss function

Published

2020

29. Host Genetic Analysis of Pulmonary NTM Disease and Non-CF Bronchietasis

Author

Takahiro Asami, Shoji Suzuki, Makoto Ishii, Kenjiro Kosaki, Hee Jae Huh, Hiroaki Matsubara, Atsuyuki Kurashima, Eva P. Szymanski, S.M. Holland, Takanori Asakura, S. Matsuda, Katsura Emoto, Junko Hamamoto, Kozo Morimoto, H.-H. Won, Surakameth Mahasirimongkol, Byung Woo Jhun, Mitsunori Yoshida, Y. Sasaki, Hervé Tettelin, Michael R. Knowles, Kenneth N. Olivier, Maimoona B Zariwala, Ho Namkoong, Yoshihiko Hoshino, Hidekatsu Yanai, Naoki Hasegawa, Manabu Ato, Tetsuya Shiomi, Yosuke Omae, Su Young Kim, Andrew J. Oler, Tomoyasu Nishimura, Hisato Shimada, Katsushi Tokunaga, L.A. Daniels, Hong Dang, Kazuma Yagi, Isano Hase, and Won-Jung Koh

Subjects

Genetics, Host (biology), Disease, Biology, Genetic analysis

Published

2020

30. Low Levels of Correctly Spliced CCDC114 Mitigate Disease Severity in Primary Ciliary Dyskinesia

Author

L.A. Daniels, Maimoona B Zariwala, A.J. Smith, Ximena M. Bustamante-Marin, Michael R. Knowles, Weining Yin, Patrick R. Sears, and Lawrence E. Ostrowski

Subjects

medicine.medical_specialty, Disease severity, business.industry, Internal medicine, medicine, medicine.disease, business, Gastroenterology, Primary ciliary dyskinesia

Published

2020

31. Investigating the Role of SPAG1 in the Cytoplasmic Assembly of Axonemal Dynein Arms: Genotypic and Phenotypic Variability of SPAG1 Mutations in Primary Ciliary Dyskinesia

Author

Margaret W. Leigh, A.J. Smith, Ximena M. Bustamante-Marin, Michael R. Knowles, Patrick R. Sears, Maimoona A. Zariwala, Lawrence E. Ostrowski, Laura E. Herring, and Weining Yin

Subjects

Cytoplasm, Genotype, medicine, Axonemal dynein, Biology, medicine.disease, Phenotype, Cell biology, Primary ciliary dyskinesia

Published

2020

32. An Official American Thoracic Society Workshop Report: Translational Research in Rare Respiratory Diseases

Author

Jennifer S. Landry, Qutayba Hamid, Lisa R. Young, Francis X. McCormack, Arnold S. Kristof, Basil J. Petrof, Frank Rauch, Maimoona A. Zariwala, Benjamin Smith, David Y. Thomas, Joel Moss, Adam J. Shapiro, Ivan O. Rosas, Alex MacKenzie, Martin Kolb, Bruce C. Trapnell, and Inga J. Murawski

Subjects

Lung Diseases, Pulmonary and Respiratory Medicine, medicine.medical_specialty, Pathology, Consensus Development Conferences as Topic, Alternative medicine, Translational research, Policy initiatives, Translational Research, Biomedical, Mice, 03 medical and health sciences, Rare Diseases, 0302 clinical medicine, Health care, medicine, Animals, Humans, 030212 general & internal medicine, Clinical care, Genetic Association Studies, Societies, Medical, American Thoracic Society Documents, Clinical Trials as Topic, Medical education, Heterogeneous group, business.industry, Molecular pathogenesis, United States, Clinical research, 030228 respiratory system, business

Abstract

Rare respiratory diseases (RRDs) are a heterogeneous group of disorders that collectively represent a significant health care burden. In recent years, strong advocacy and policy initiatives have led to advances in the implementation of research and clinical care for rare diseases. The development of specialized centers and research networks has facilitated support for affected individuals as well as emerging programs in basic, translational, and clinical research. In selected RRDs, subsequent gains in knowledge have informed the development of targeted therapies and effective diagnostic tests, but many gaps persist. There was therefore a desire to identify the elements contributing to an effective translational research program in RRDs. To this end, a workshop was convened in October 2015 with a focus on the implementation of effective transnational research networks and collaborations aimed at developing novel diagnostic and therapeutic tools. Key elements included an emphasis on molecular pathogenesis, the continuing engagement of patient advocacy groups and policy makers, the effective use of preclinical models in the translational research pipeline, and the detailed phenotyping of patient cohorts. During the course of the workshop, current logistical and knowledge gaps were identified, and new solutions or opportunities were highlighted.

Published

2017

33. De Novo Mutations in FOXJ1 Result in a Motile Ciliopathy with Hydrocephalus and Randomization of Left/Right Body Asymmetry

Author

Christian Vogelberg, Tabea Nöthe-Menchen, Heike Olbrich, Angela Brentrup, Margaret W. Leigh, Julia Wallmeier, Heymut Omran, Thomas Kaiser, Stephanie D. Davis, Thomas W. Ferkol, Deborah J. Morris-Rosendahl, Henrike Krenz, Sandra Cindric, Diana Frank, Siobhán B. Carr, Michael R. Knowles, Niki T. Loges, Claire Hogg, Isabella Aprea, Holger Thiele, Susan K. Dutcher, Hannah M. Mitchison, Petra Pennekamp, Gerard W. Dougherty, Maimoona A. Zariwala, Amelia Shoemark, Marius Wöste, Frank Ahrens, Janine Altmüller, and Jeffrey J. Atkinson

Subjects

0301 basic medicine, Ependymal Cell, Video microscopy, Biology, Cerebral Ventricles, 03 medical and health sciences, 0302 clinical medicine, Cerebrospinal fluid, Ciliogenesis, Report, Ependyma, Genetics, medicine, Humans, Cilia, Genetics (clinical), Cilium, Body movement, Epithelial Cells, Forkhead Transcription Factors, medicine.disease, Basal Bodies, Ciliopathies, Cell biology, Ciliopathy, 030104 developmental biology, Mutation, Motile cilium, 030217 neurology & neurosurgery, Hydrocephalus

Abstract

Hydrocephalus is one of the most prevalent form of developmental central nervous system (CNS) malformations. Cerebrospinal fluid (CSF) flow depends on both heartbeat and body movement. Furthermore, it has been shown that CSF flow within and across brain ventricles depends on cilia motility of the ependymal cells lining the brain ventricles, which play a crucial role to maintain patency of the narrow sites of CSF passage during brain formation in mice. Using whole-exome and whole-genome sequencing, we identified an autosomal-dominant cause of a distinct motile ciliopathy related to defective ciliogenesis of the ependymal cilia in six individuals. Heterozygous de novo mutations in FOXJ1, which encodes a well-known member of the forkhead transcription factors important for ciliogenesis of motile cilia, cause a motile ciliopathy that is characterized by hydrocephalus internus, chronic destructive airway disease, and randomization of left/right body asymmetry. Mutant respiratory epithelial cells are unable to generate a fluid flow and exhibit a reduced number of cilia per cell, as documented by high-speed video microscopy (HVMA), transmission electron microscopy (TEM), and immunofluorescence analysis (IF). TEM and IF demonstrate mislocalized basal bodies. In line with this finding, the focal adhesion protein PTK2 displays aberrant localization in the cytoplasm of the mutant respiratory epithelial cells.

Published

2019

34. Mutation ofCFAP57causes primary ciliary dyskinesia by disrupting the asymmetric targeting of a subset of ciliary inner dynein arms

Author

Maimoona A. Zariwala, Ximena M. Bustamante-Marin, Mathieu Bottier, Mihaela Stoyanova, Michael R. Knowles, Patrick R. Sears, Hailey Bowen, Amjad Horani, Lawrence E. Ostrowski, Donald F. Conrad, Susan K. Dutcher, Wu Lin Charng, and L.A. Daniels

Subjects

0303 health sciences, Cilium, Dynein, Flagellum, Biology, medicine.disease, Cell biology, 03 medical and health sciences, Ciliopathy, 0302 clinical medicine, Microtubule, Motile cilium, medicine, Inner dynein arm assembly, 030217 neurology & neurosurgery, 030304 developmental biology, Primary ciliary dyskinesia

Abstract

Primary ciliary dyskinesia (PCD) is characterized by chronic airway disease, male infertility, and randomization of the left/right body axis, and is caused by defects of motile cilia and sperm flagella. We screened a cohort of affected individuals that lack an obvious TEM structural phenotype for pathogenic variants using whole exome capture and next generation sequencing. The population sampling probability (PSAP) algorithm identified one subject with a homozygous nonsense variant [(c.1762C>T) p.(Arg588*) exon 11] in the uncharacterizedCFAP57gene. In normal human nasal epithelial cells, CFAP57 localizes throughout the ciliary axoneme. Analysis of cells from the PCD patient shows a loss of CFAP57, reduced beat frequency, and an alteration in the ciliary waveform. Knockdown ofCFAP57in human tracheobronchial epithelial cells (hTECs) recapitulates these findings. Phylogenetic analysis showed that CFAP57 is conserved in organisms that assemble motile cilia, andCFAP57is allelic with theBOP2gene identified previously inChlamydomonas. Two independent, insertionalfap57 Chlamydomonasmutant strains show reduced swimming velocity and altered waveforms. Tandem mass spectroscopy showed that CFAP57 is missing, and the “g” inner dyneins (DHC7 and DHC3) and the “d” inner dynein (DHC2) are reduced. Our data demonstrate that the FAP57 protein is required for the asymmetric assembly of inner dyneins on only a subset of the microtubule doublets, and this asymmetry is essential for the generation of an effective axonemal waveform. Together, our data identifies mutations inCFAP57as a cause of PCD with a specific defect in the inner dynein arm assembly process.SignificanceMotile cilia are found throughout eukaryotic organisms and performs essential functions. Primary ciliary dyskinesia (PCD) is a rare disease that affects the function of motile cilia. By applying a novel population sampling probability algorithm (PSAP) that uses large population sequencing databases and pathogenicity prediction algorithms, we identified a variant in an uncharacterized gene,CFAP57. This is the first reported example of PCD caused by a mutation that affects only a subset of the inner dynein arms, which are needed to generate the waveform. CFAP57 identifies an address for specific dynein arms. These findings demonstrate the effectiveness of the PSAP algorithm, expand our understanding of the positioning of dynein arms, and identify mutations inCFAP57as a cause of PCD.

Published

2019

35. Cytoplasmic 'ciliary inclusions' in isolation are not sufficient for the diagnosis of primary ciliary dyskinesia

Author

Maimoona A. Zariwala, Scott D. Sagel, Kelli M. Sullivan, Susan K. Dutcher, Margaret W. Leigh, Kimberlie A. Burns, Timothy J. Vece, Michael R. Knowles, and Roman Yusupov

Subjects

Pulmonary and Respiratory Medicine, Male, Pathology, medicine.medical_specialty, Mucociliary clearance, Nitric Oxide, 03 medical and health sciences, 0302 clinical medicine, Clinical history, 030225 pediatrics, Exome Sequencing, otorhinolaryngologic diseases, medicine, Humans, Cilia, Genetic Testing, Genetic testing, Primary ciliary dyskinesia, medicine.diagnostic_test, business.industry, Cilium, Infant, medicine.disease, Situs inversus, Low nasal nitric oxide, Nasal Mucosa, 030228 respiratory system, Cytoplasm, Child, Preschool, Pediatrics, Perinatology and Child Health, Female, business, Ciliary Motility Disorders

Abstract

Background The diagnosis of primary ciliary dyskinesia (PCD) is difficult and requires a combination of clinical features, nasal nitric oxide testing, cilia ultrastructural analysis by electron microscopy (EM), and genetics. A recently described cytoplasmic ultrastructural change termed "ciliary inclusions" was reported to be diagnostic of PCD; however, no supporting evidence of PCD was provided. In this study, we sought to confirm, or refute, the diagnosis of PCD in subjects with "ciliary inclusions" on EM. Methods Six subjects from five families with previous lab reports of "ciliary inclusions" on EMs of ciliated cells were identified and evaluated at a Genetic Disorders of Mucociliary Clearance Consortium site. We performed a detailed clinical history, nasal nitric oxide measurement, genetic testing including whole-exome sequencing (WES), and when possible, repeat ciliary EM study. Results Only one of six subjects had multiple and persistent clinical features congruent with PCD. No subject had situs inversus. Only one of six subjects had a very low nasal nitric oxide level. No "ciliary inclusions" were found in three subjects who had a repeat ciliary EM, and ciliary axonemal ultrastructures were normal. Genetic testing, including WES, was negative for PCD-causing genes, and for pathogenic variants in gene pathways that might cause "ciliary inclusions," such as ciliary biogenesis. Conclusion "Ciliary Inclusions", in isolation, are not sufficient to diagnosis PCD. If seen, additional studies should be done to pursue an accurate diagnosis.

Published

2019

36. Nasal Nitric Oxide in Primary Immunodeficiency and Primary Ciliary Dyskinesia: Helping to Distinguish Between Clinically Similar Diseases

Author

Keith R. Nykamp, Reza Alizadehfar, Zofia N. Zysman-Colman, Maimoona A. Zariwala, Kimberley R. Kaspy, Adam J. Shapiro, Michael R. Knowles, and Donald C. Vinh

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Adolescent, Mucociliary clearance, Primary Immunodeficiency Diseases, Immunology, Nasal congestion, Nose, Nitric Oxide, Article, Nitric oxide, Diagnosis, Differential, 03 medical and health sciences, chemistry.chemical_compound, Young Adult, 0302 clinical medicine, Medical microbiology, Internal medicine, otorhinolaryngologic diseases, Immunology and Allergy, Medicine, Humans, Child, Primary ciliary dyskinesia, Respiratory tract infections, business.industry, Neonatal respiratory distress, Middle Aged, medicine.disease, respiratory tract diseases, 030104 developmental biology, chemistry, Primary immunodeficiency, Female, medicine.symptom, business, 030215 immunology, Ciliary Motility Disorders

Abstract

PURPOSE: Primary Ciliary Dyskinesia (PCD) is a rare disorder of mucociliary clearance leading to recurrent upper and lower respiratory tract infections. PCD is difficult to clinically distinguish from other entities leading to recurrent oto-sino-pulmonary infections, including primary immunodeficiency (PID). Nasal nitric oxide (nNO) is a sensitive and specific diagnostic test for PCD, but it has not been thoroughly examined in PID. Past publications have suggested an overlap in nNO levels among subjects with PCD and PID. We sought to determine if nNO measurements among patients diagnosed with PID would fall significantly above the established PCD diagnostic cutoff value of 77 nL/min. METHODS: Children >5 years old and adults with definitive PID or PCD diagnoses were recruited from outpatient subspecialty clinics. Participants underwent nNO testing by standardized protocol using a chemiluminiescence analyzer and completed a questionnaire concerning their chronic oto-sino-pulmonary symptoms, including key clinical criteria specific to diagnosed PCD (neonatal respiratory distress at term birth, year-round cough or nasal congestion starting before 6 months of age, any organ laterality defect). RESULTS: Participants included 32 patients with PID, 27 patients with PCD and 19 healthy controls. Median nNO was 228.9.1 nL/min in the PID group, 19.7 nL/min in the PCD group and 269.4 in the healthy controls (p

Published

2019

37. Primary Ciliary Dyskinesia

Author

Maimoona B Zariwala, Michael R. Knowles, and Margaret W. Leigh

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, Pathology, medicine.medical_specialty, Heterotaxy Syndrome, Nasal congestion, Nitric Oxide, Article, 03 medical and health sciences, 0302 clinical medicine, Adrenal Cortex Hormones, Administration, Inhalation, otorhinolaryngologic diseases, Humans, Medicine, Cilia, Genetic Testing, Radial spoke head 1 homolog, Sinusitis, Administration, Intranasal, Primary ciliary dyskinesia, Saline Solution, Hypertonic, Respiratory Distress Syndrome, Newborn, Kartagener Syndrome, business.industry, Cilium, Endoscopy, respiratory system, Situs Inversus, medicine.disease, Middle Ear Ventilation, Anti-Bacterial Agents, respiratory tract diseases, Otitis Media, Situs inversus, Phenotype, 030104 developmental biology, Breath Tests, Cough, 030228 respiratory system, Chronic Disease, Nasal Lavage, Motile cilium, medicine.symptom, business

Abstract

Primary ciliary dyskinesia (PCD) is a recessive genetically heterogeneous disorder of motile cilia with chronic otosinopulmonary disease and organ laterality defects in ∼50% of cases. The prevalence of PCD is difficult to determine. Recent diagnostic advances through measurement of nasal nitric oxide and genetic testing has allowed rigorous diagnoses and determination of a robust clinical phenotype, which includes neonatal respiratory distress, daily nasal congestion, and wet cough starting early in life, along with organ laterality defects. There is early onset of lung disease in PCD with abnormal airflow mechanics and radiographic abnormalities detected in infancy and early childhood.

Published

2016

38. Author Correction: A human ciliopathy reveals essential functions for NEK10 in airway mucociliary clearance

Author

Hanan E. Shamseldin, Jason H. Yang, Guillermo J. Tearney, Martin S. Taylor, Gerard W. Dougherty, Raghu R. Chivukula, Daniel T. Montoro, Johnny L. Carson, Heymut Omran, Evgeni M. Frenkel, M. Leigh Anne Daniels, David M. Sabatini, Ibrahim Almogarri, Lida P. Hariri, Michael R. Knowles, Hui Min Leung, Fowzan S. Alkuraya, Katharine E. Black, Maimoona A. Zariwala, Vladimir Vinarsky, and Patrick R. Sears

Subjects

Adult, Adolescent, Proteome, Mucociliary clearance, Respiratory System, Cystic Fibrosis Transmembrane Conductance Regulator, Cell Separation, Article, General Biochemistry, Genetics and Molecular Biology, Young Adult, medicine, Humans, NIMA-Related Kinases, Exome, Microscopy, Phase-Contrast, Child, Microscopy, Video, business.industry, Homozygote, Epithelial Cells, X-Ray Microtomography, General Medicine, Flow Cytometry, medicine.disease, Ciliopathies, Ciliopathy, HEK293 Cells, Phenotype, Mucociliary Clearance, Mutation, Immunology, Female, Tomography, X-Ray Computed, Airway, business

Abstract

Mucociliary clearance, the physiological process by which mammalian conducting airways expel pathogens and unwanted surface materials from the respiratory tract, depends on the coordinated function of multiple specialized cell types, including basal stem cells, mucus-secreting goblet cells, motile ciliated cells, cystic fibrosis transmembrane conductance regulator (CFTR)-rich ionocytes, and immune cells

Published

2020

39. Primary Ciliary Dyskinesia: Longitudinal Study of Lung Disease by Ultrastructure Defect and Genotype

Author

Adam J. Shapiro, Margaret Rosenfeld, Stephanie D. Davis, Kelli M. Sullivan, Jessica E. Pittman, Sharon D. Dell, Jeffrey P. Krischer, Maimoona A. Zariwala, Keith R. Nykamp, Hye-Seung Lee, Carlos Milla, Thomas W. Ferkol, Scott D. Sagel, Michael R. Knowles, and Margaret W Leigh

Subjects

Pulmonary and Respiratory Medicine, Male, Pathology, medicine.medical_specialty, Longitudinal study, Genotype, Disease, Critical Care and Intensive Care Medicine, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, mental disorders, otorhinolaryngologic diseases, Medicine, Humans, 030212 general & internal medicine, Cilia, Longitudinal Studies, Prospective Studies, Child, Lung, Primary ciliary dyskinesia, business.industry, Kartagener Syndrome, Cilium, medicine.disease, nervous system diseases, Respiratory Function Tests, Phenotype, 030228 respiratory system, Lung disease, Mutation, Ultrastructure, Female, business

Abstract

In primary ciliary dyskinesia, factors leading to disease heterogeneity are poorly understood.To describe early lung disease progression in primary ciliary dyskinesia and identify associations between ultrastructural defects and genotypes with clinical phenotype.This was a prospective, longitudinal (5 yr), multicenter, observational study. Inclusion criteria were less than 19 years at enrollment and greater than or equal to two annual study visits. Linear mixed effects models including random slope and random intercept were used to evaluate longitudinal associations between the ciliary defect group (or genotype group) and clinical features (percent predicted FEVA total of 137 participants completed 732 visits. The group with absent inner dynein arm, central apparatus defects, and microtubular disorganization (IDA/CA/MTD) (n = 41) were significantly younger at diagnosis and in mixed effects models had significantly lower percent predicted FEVParticipants with IDA/MTD/CA defects, which included individuals with CCDC39 or CCDC40 mutations, had worse lung function and growth indices compared with those with outer dynein arm defects and DNAH5 mutations, respectively. The only group with a significant lung function decline over time were participants with IDA/MTD/CA defects.

Published

2018

40. The prevalence of the defining features of primary ciliary dyskinesia within a cri du chat syndrome cohort

Author

Karen E. Weck, Margaret W. Leigh, Michael R. Knowles, Dennis J. Campbell, Catherine D. Sanders, Maimoona A. Zariwala, Kay C. Chao, Adam J. Shapiro, Whitney E. Wolf, and Ian F. G. King

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, Cri-du-Chat Syndrome, Male, medicine.medical_specialty, animal structures, Cri du chat, Adolescent, Cri du Chat Syndrome, Comorbidity, Nasal congestion, Cohort Studies, 03 medical and health sciences, Microscopy, Electron, Transmission, Internal medicine, otorhinolaryngologic diseases, medicine, Prevalence, Humans, Child, Genetic testing, Primary ciliary dyskinesia, medicine.diagnostic_test, business.industry, medicine.disease, Dysphagia, Hypotonia, respiratory tract diseases, 030104 developmental biology, Child, Preschool, Pediatrics, Perinatology and Child Health, Cohort, Female, medicine.symptom, business, Ciliary Motility Disorders

Abstract

Background Primary ciliary dyskinesia (PCD) and cri du chat syndrome (CdCS) are distinct disorders that can co-occur due to a common genetic locus on chromosome 5p. Chronic respiratory symptoms associated with PCD can occur in CdCS and are typically attributed to hypotonia, dysphagia, and aspiration. The prevalence of PCD among individuals with CdCS is not known. Methods An online survey assessing common features of PCD was distributed to members of the 5P Minus Society, a cri du chat patient advocacy group. Respondents who met criteria for elevated risk of PCD (at least 3 symptoms or other features highly suggestive of PCD) were offered PCD genetic testing. Results For the 123 respondents (median age 10.1 years with IQR 5.5-17.3 years; from 33 U.S. states and 10 other countries) chronic respiratory symptoms associated with PCD were prevalent, including unexplained neonatal respiratory distress, year-round nasal congestion beginning in infancy, and year-round, wet cough beginning in infancy in 35%, 32%, and 20% of respondents, respectively. Fifteen respondents (12%) met criteria for elevated risk for PCD and completed genetic analysis; however, none were diagnostic for PCD. A PCD clinical center evaluated an additional subject with CdCS who met criteria for likely PCD and had negative genetics, but had diagnostic electron microscopy of the respiratory cilia (missing outer dynein arms). Conclusion Clinicians should be aware of the genetic connection between CdCS and PCD. Non-informative genetic testing does not rule out PCD. CdCS patients with chronic respiratory symptoms may benefit from referral to specialized PCD diagnostic centers.

Published

2018

41. Diagnosis of primary ciliary dyskinesia: An official American thoracic society clinical practice guideline

Author

M. Leigh Anne Daniels, Scott D. Sagel, Deepika Polineni, Lynn Ehrne, Sam J. Daniel, Matthew L. Cooper, Maimoona A. Zariwala, Michele Manion, Margaret Rosenfeld, Thomas W. Ferkol, Billy Anton, Valery Lavergne, Stephanie M. Ware, Maureen B. Josephson, Jessica E. Pittman, Elena Guadagno, Lawrence M. Nogee, Sharon D. Dell, Michael R. Knowles, Mark A. Chilvers, Margaret W. Leigh, Stephanie D. Davis, Carlos Milla, Marcus Herbert Jones, Ibrahim A. Janahi, Ozge Yilmaz, Lucy Morgan, Tori Eastvold, Kenneth N. Olivier, and Adam J. Shapiro

Subjects

Pulmonary and Respiratory Medicine, medicine.medical_specialty, Critical Care and Intensive Care Medicine, Sensitivity and Specificity, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Multidisciplinary approach, medicine, Humans, Genetic Predisposition to Disease, Medical physics, Cilia, Prospective Studies, 030212 general & internal medicine, Grading (education), Diagnostic Techniques and Procedures, Societies, Medical, Retrospective Studies, Primary ciliary dyskinesia, Kartagener Syndrome, business.industry, Diagnostic test, Guideline, medicine.disease, United States, ATS Clinical Practice Guideline, Clinical Practice, Cross-Sectional Studies, Systematic review, 030228 respiratory system, Practice Guidelines as Topic, business

Abstract

Background: This document presents the American Thoracic Society clinical practice guidelines for the diagnosis of primary ciliary dyskinesia (PCD). Target Audience: Clinicians investigating adult and pediatric patients for possible PCD. Methods: Systematic reviews and, when appropriate, meta-Analyses were conducted to summarize all available evidence pertinent to our clinical questions. Evidence was assessed using the GRADE (Grading of Recommendations, Assessment, Development and Evaluation) approach for diagnosis and discussed by amultidisciplinary panelwith expertise in PCD. Predetermined conflict-of-interest management strategies were applied, and recommendations were formulated, written, and graded exclusively by the nonconflicted panelists. Three conflicted individuals were also prohibited from writing, editing, or providing feedback on the relevant sections of the manuscript. Results: After considering diagnostic test accuracy, confidence in the estimates for each diagnostic test, relative importance of test results studied, desirable and undesirable direct consequences of each diagnostic test, downstream consequences of each diagnostic test result, patient values and preferences, costs, feasibility, acceptability, and implications for health equity, the panel made recommendations for or against the use of specific diagnostic tests as compared with using the current reference standard (transmission electron microscopy and/or genetic testing) for the diagnosis of PCD. Conclusions: The panel formulated and provided a rationale for the direction as well as for the strength of each recommendation to establish the diagnosis of PCD.

Published

2018

42. Diagnosis, monitoring, and treatment of primary ciliary dyskinesia: PCD foundation consensus recommendations based on state of the art review

Author

Margaret W. Leigh, Carlos Milla, Sam J. Daniel, Maimoona A. Zariwala, Adam J. Kimple, Sharon D. Dell, Adam J. Shapiro, Scott D. Sagel, Margaret Rosenfeld, Michael R. Knowles, Michele Manion, Kenneth N. Olivier, Thomas W. Ferkol, and Stephanie D. Davis

Subjects

Pulmonary and Respiratory Medicine, Pediatrics, medicine.medical_specialty, Respiratory Therapy, animal structures, PCD, kartagener, Biopsy, primary ciliary dyskinesia, consensus statement, Disease, PCD Foundation, Pneumococcal Vaccines, 03 medical and health sciences, 0302 clinical medicine, medicine, otorhinolaryngologic diseases, Respiratory Syncytial Virus Vaccines, Humans, 030212 general & internal medicine, Genetic Testing, Disease management (health), Genetic testing, Primary ciliary dyskinesia, Microscopy, Video, medicine.diagnostic_test, business.industry, Kartagener Syndrome, Foundation (evidence), Disease Management, medicine.disease, State of the Art, 3. Good health, Review article, respiratory tract diseases, Clinical trial, Microscopy, Electron, 030228 respiratory system, Breath Tests, Influenza Vaccines, Pediatrics, Perinatology and Child Health, Chronic Disease, North America, Differential diagnosis, business

Abstract

Summary Primary ciliary dyskinesia (PCD) is a genetically heterogeneous, rare lung disease resulting in chronic oto‐sino‐pulmonary disease in both children and adults. Many physicians incorrectly diagnose PCD or eliminate PCD from their differential diagnosis due to inexperience with diagnostic testing methods. Thus far, all therapies used for PCD are unproven through large clinical trials. This review article outlines consensus recommendations from PCD physicians in North America who have been engaged in a PCD centered research consortium for the last 10 years. These recommendations have been adopted by the governing board of the PCD Foundation to provide guidance for PCD clinical centers for diagnostic testing, monitoring, and appropriate short and long‐term therapeutics in PCD patients. Pediatr Pulmonol. 2016;51:115–132. © 2015 The Authors. Pediatric Pulmonology Published by Wiley Periodicals, Inc.

Published

2015

43. Whole-Exome Sequencing and Targeted Copy Number Analysis in Primary Ciliary Dyskinesia

Author

Tara Paton, Maimoona A. Zariwala, Peter N. Ray, Tracy Stockley, Sharon D. Dell, Michael R. Knowles, David A. Hall, Rebekah Jobling, Lynette Lau, Stephen W. Scherer, Christian R. Marshall, and Raymond H. Kim

Subjects

Male, primary ciliary dyskinesia, Bioinformatics, 0302 clinical medicine, Exome, whole-exome sequencing, Copy-number variation, Child, Frameshift Mutation, Genetics (clinical), Exome sequencing, Primary ciliary dyskinesia, Sanger sequencing, Genetics, 0303 health sciences, copy number variation, High-Throughput Nucleotide Sequencing, Nuclear Proteins, 3. Good health, Codon, Nonsense, Child, Preschool, symbols, Ciliary Motility Disorders, Female, Microtubule-Associated Proteins, Algorithms, Adult, Adolescent, DNA Copy Number Variations, Copy number analysis, Nerve Tissue Proteins, Investigations, Biology, diagnostic testing, 03 medical and health sciences, symbols.namesake, otorhinolaryngologic diseases, medicine, Humans, Molecular Biology, 030304 developmental biology, Genome, Human, Genetic heterogeneity, Infant, Axonemal Dyneins, Sequence Analysis, DNA, medicine.disease, Cytoskeletal Proteins, 030228 respiratory system

Abstract

Primary ciliary dyskinesia (PCD) is an autosomal-recessive disorder resulting from loss of normal ciliary function. Symptoms include neonatal respiratory distress, chronic sinusitis, bronchiectasis, situs inversus, and infertility. Clinical features may be subtle and highly variable, making the diagnosis of PCD challenging. The diagnosis can be confirmed with ciliary ultrastructure analysis and/or molecular genetic testing of 32 PCD-associated genes. However, because of this genetic heterogeneity, comprehensive molecular genetic testing is not considered the standard of care, and the most efficient molecular approach has yet to be elucidated. Here, we propose a cost-effective and time-efficient molecular genetic algorithm to solve cases of PCD. We conducted targeted copy number variation (CNV) analysis and/or whole-exome sequencing on 20 families (22 patients) from a subset of 45 families (52 patients) with a clinical diagnosis of PCD who did not have a molecular genetic diagnosis after Sanger sequencing of 12 PCD-associated genes. This combined molecular genetic approach led to the identification of 4 of 20 (20%) families with clinically significant CNVs and 7 of 20 (35%) families with biallelic pathogenic mutations in recently identified PCD genes, resulting in an increased molecular genetic diagnostic rate of 55% (11/20). In patients with a clinical diagnosis of PCD, whole-exome sequencing followed by targeted CNV analysis results in an overall molecular genetic yield of 76% (34/45).

Published

2015

44. PRIMARY CILIARY DYSKINESIA: KEEP IT ON YOUR RADAR

Author

Maimoona A. Zariwala, Lawrence E. Ostrowski, and Margaret Rosenfeld

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, Adult, Male, Pediatrics, medicine.medical_specialty, Adolescent, Consanguinity, Disease, medicine.disease_cause, Cystic fibrosis, Article, Cohort Studies, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Asian People, otorhinolaryngologic diseases, Medicine, Missense mutation, Humans, Pakistan, Child, Primary ciliary dyskinesia, Mutation, business.industry, Genetic heterogeneity, Kartagener Syndrome, medicine.disease, United Kingdom, 030104 developmental biology, 030228 respiratory system, Child, Preschool, Cohort, Female, business, Microtubule-Associated Proteins

Abstract

Primary ciliary dyskinesia (PCD) is a rare disorder of mucociliary clearance resulting in chronic oto-sinopulmonary disease. While the prevalence worldwide is estimated to be 1:10 000–1:15 000, it may be much higher in certain communities, especially where consanguinity is more prevalent. In the British South Asian community, for example, the prevalence has been estimated at 1:2450, similar to that of cystic fibrosis among caucasians.1 In Thorax , Shoemark and colleagues2 describe PCD in a highly consanguineous UK South Asian community, due to homozygous missense variants in CCDC103, usually resulting in the loss of both outer and inner dynein arms. The investigators identified 86 patients of South Asian (primarily Pakistani) descent with clinical signs and symptoms of PCD from the UK National PCD Diagnostic and Management Services. These individuals had a compatible clinical phenotype, but diagnosis was complicated by the fact that many of the standard diagnostic tests for PCD had yielded variable and frequently normal results, including nasal nitric oxide, ciliary beat frequency and ciliary ultrastructure by transmission electron microscopy. Ultimately, next-generation sequencing confirmed a homozygous pathogenic variant, p.His154Pro, in CCDC103 in 16 (19%) of these 86 cases, from 12 independent families. From a clinical perspective, this report by Shoemark and colleagues2 highlights two important issues in the diagnosis of PCD. The first is that the prevalence of PCD may be higher than previously appreciated in certain populations, particularly in highly consanguineous communities. Indeed, in this report, all 16 patients with homozygous CCDC103 p.His154Pro mutations were children of consanguineous parents. While this UK South Asian PCD cohort was enriched for the CCDC103 p.His154Pro mutation, a number of other PCD-causing mutations were also present, including CCDC40 , DNAAF1 , HEATR2 , LRRC6 , ZMYND10 and RSPH4A . A high prevalence of PCD with genetic heterogeneity has similarly been …

Published

2017

45. Carrier frequencies of eleven mutations in eight genes associated with primary ciliary dyskinesia in the Ashkenazi Jewish population

Author

Michael R. Knowles, Anastasia Fedick, Chaim Jalas, Nathan R. Treff, and Maimoona A. Zariwala

Subjects

carrier frequency, Population, primary ciliary dyskinesia, situs inversus, Male infertility, otorhinolaryngologic diseases, Genetics, Medicine, education, Molecular Biology, Genetics (clinical), Primary ciliary dyskinesia, education.field_of_study, Kartagener syndrome, business.industry, Genetic heterogeneity, Kartagener Syndrome, Original Articles, medicine.disease, 3. Good health, Situs inversus, Ashkenazi, Mutation (genetic algorithm), Motile cilium, business

Abstract

Primary ciliary dyskinesia (PCD) is a genetically heterogeneous, autosomal recessive disorder that results from functional and ultrastructural abnormalities of motile cilia. Patients with PCD have diverse clinical phenotypes that include chronic upper and lower respiratory tract infections, situs inversus, heterotaxy with or without congenital heart disease, and male infertility, among others. In this report, the carrier frequencies for eleven mutations in eight PCD-associated genes (DNAI1, DNAI2, DNAH5, DNAH11, CCDC114, CCDC40, CCDC65, and C21orf59) that had been found in individuals of Ashkenazi Jewish descent were investigated in order to advise on including them in existing clinical mutation panels for this population. Results showed relatively high carrier frequencies for the DNAH5 c.7502G>C mutation (0.58%), the DNAI2 c.1304G>A mutation (0.50%), and the C21orf59 c.735C>G mutation (0.48%), as well as lower frequencies for mutations in DNAI1, CCDC65, CCDC114, and DNAH11 (0.10–0.29%). These results suggest that several of these genes should be considered for inclusion in carrier screening panels in the Ashkenazi Jewish population.

Published

2014

46. Laterality Defects Other Than Situs Inversus Totalis in Primary Ciliary Dyskinesia

Author

Kimberlie A. Burns, Maimoona A. Zariwala, Margaret W. Leigh, Adam J. Shapiro, Milan J. Hazucha, Margaret Rosenfeld, Thomas W. Ferkol, Blair V. Robinson, Michael R. Knowles, Sharon D. Dell, Whitney E. Wolf, Kenneth N. Olivier, Johnny L. Carson, Carlos Milla, Scott D. Sagel, and Stephanie D. Davis

Subjects

Pulmonary and Respiratory Medicine, medicine.medical_specialty, business.industry, Situs ambiguus, Kartagener Syndrome, Anatomy, Gene mutation, Critical Care and Intensive Care Medicine, medicine.disease, Gastroenterology, Situs inversus, medicine.anatomical_structure, Internal medicine, otorhinolaryngologic diseases, medicine, Motile cilium, Cardiology and Cardiovascular Medicine, business, Heterotaxy, Situs solitus, Primary ciliary dyskinesia

Abstract

BACKGROUND Motile cilia dysfunction causes primary ciliary dyskinesia (PCD), situs inversus totalis (SI), and a spectrum of laterality defects, yet the prevalence of laterality defects other than SI in PCD has not been prospectively studied. METHODS In this prospective study, participants with suspected PCD were referred to our multisite consortium. We measured nasal nitric oxide (nNO) level, examined cilia with electron microscopy, and analyzed PCD-causing gene mutations. Situs was classified as (1) situs solitus (SS), (2) SI, or (3) situs ambiguus (SA), including heterotaxy. Participants with hallmark electron microscopic defects, biallelic gene mutations, or both were considered to have classic PCD. RESULTS Of 767 participants (median age, 8.1 years, range, 0.1-58 years), classic PCD was defined in 305, including 143 (46.9%), 125 (41.0%), and 37 (12.1%) with SS, SI, and SA, respectively. A spectrum of laterality defects was identified with classic PCD, including 2.6% and 2.3% with SA plus complex or simple cardiac defects, respectively; 4.6% with SA but no cardiac defect; and 2.6% with an isolated possible laterality defect. Participants with SA and classic PCD had a higher prevalence of PCD-associated respiratory symptoms vs SA control participants (year-round wet cough, P P = .015; neonatal respiratory distress, P = .009; digital clubbing, P = .021) and lower nNO levels (median, 12 nL/min vs 252 nL/min; P CONCLUSIONS At least 12.1% of patients with classic PCD have SA and laterality defects ranging from classic heterotaxy to subtle laterality defects. Specific clinical features of PCD and low nNO levels help to identify PCD in patients with laterality defects. TRIAL REGISTRY ClinicalTrials.gov ; No.: NCT00323167; URL: www.clinicaltrials.gov

Published

2014

47. The prevalence of clinical features associated with primary ciliary dyskinesia in a heterotaxy population: results of a web-based survey

Author

Adam J. Shapiro, Maimoona A. Zariwala, Margaret W. Leigh, Michael R. Knowles, and Sue Tolleson-Rinehart

Subjects

Adult, Male, Canada, Pediatrics, medicine.medical_specialty, Adolescent, Population, Heterotaxy Syndrome, Article, Young Adult, mental disorders, Prevalence, otorhinolaryngologic diseases, medicine, Humans, Respiratory system, Young adult, Child, education, Primary ciliary dyskinesia, Internet, education.field_of_study, Bronchiectasis, Kartagener Syndrome, business.industry, Cilium, Australia, Infant, General Medicine, Middle Aged, medicine.disease, Health Surveys, United Kingdom, United States, nervous system diseases, Child, Preschool, Pediatrics, Perinatology and Child Health, Female, Cardiology and Cardiovascular Medicine, business, Ireland, Heterotaxy

Abstract

Primary ciliary dyskinesia and heterotaxy are rare but not mutually exclusive disorders, which result from cilia dysfunction. Heterotaxy occurs in at least 12.1% of primary ciliary dyskinesia patients, but the prevalence of primary ciliary dyskinesia within the heterotaxy population is unknown. We designed and distributed a web-based survey to members of an international heterotaxy organisation to determine the prevalence of respiratory features that are common in primary ciliary dyskinesia and that might suggest the possibility of primary ciliary dyskinesia. A total of 49 members (25%) responded, and 37% of the respondents have features suggesting the possibility of primary ciliary dyskinesia, defined as (1) the presence of at least two chronic respiratory symptoms, or (2) bronchiectasis or history of respiratory pathogens suggesting primary ciliary dyskinesia. Of the respondents, four completed comprehensive, in-person evaluations, with definitive primary ciliary dyskinesia confirmed in one individual, and probable primary ciliary dyskinesia identified in two others. The high prevalence of respiratory features compatible with primary ciliary dyskinesia in this heterotaxy population suggests that a subset of heterotaxy patients have dysfunction of respiratory, as well as embryonic nodal cilia. To better assess the possibility of primary ciliary dyskinesia, heterotaxy patients with chronic oto-sino-respiratory symptoms should be referred for a primary ciliary dyskinesia evaluation.

Published

2014

48. Mutations in RSPH1 Cause Primary Ciliary Dyskinesia with a Unique Clinical and Ciliary Phenotype

Author

Hilda M. Metjian, Whitney E. Wolf, Jay Shendure, Michael V. Patrone, Peadar G. Noone, Michael R. Knowles, Hye-Seung Lee, Thomas W. Ferkol, Patrick R. Sears, Martin Kircher, Scott D. Sagel, Jeffrey P. Krischer, Peter J. Noone, Jan Halbritter, Deborah A. Nickerson, Edgar A. Otto, Sharon D. Dell, Lawrence E. Ostrowski, Aruna Sannuti, Friedhelm Hildebrandt, Maimoona A. Zariwala, Margaret Rosenfeld, Hong Dang, Michael J. Bamshad, Scott H. Randell, Kenneth N. Olivier, Johnny L. Carson, Carlos Milla, Christina A. Olson, Milan J. Hazucha, Weining Yin, Stephanie D. Davis, Toby W. Hurd, Heon Yung Gee, Stefan Kohl, and Margaret W Leigh

Subjects

Adult, Genetic Markers, Male, Pulmonary and Respiratory Medicine, animal structures, Adolescent, DNA Mutational Analysis, Biology, Critical Care and Intensive Care Medicine, medicine.disease_cause, Young Adult, otorhinolaryngologic diseases, medicine, Humans, Exome, Cilia, Genetic Testing, Child, Genetic Association Studies, Exome sequencing, Genetic testing, Primary ciliary dyskinesia, Genetics, Mutation, medicine.diagnostic_test, Kartagener Syndrome, Genetic heterogeneity, Homozygote, Sequence Analysis, DNA, Middle Aged, medicine.disease, Molecular biology, respiratory tract diseases, DNA-Binding Proteins, Nasal Mucosa, Ciliopathy, Linear Models, Motile cilium, Female, Original Article

Abstract

Rationale: Primary ciliary dyskinesia (PCD) is a genetically heterogeneous recessive disorder of motile cilia, but the genetic cause is not defined for all patients with PCD. Objectives: To identify disease-causingmutations in novel genes, we performed exome sequencing, follow-up characterization, mutation scanning, and genotype-phenotype studies in patients with PCD. Methods: Whole-exome sequencing was performed using NimbleGen capture and Illumina HiSeq sequencing. Sanger-based sequencing was used for mutation scanning, validation, and segregation analysis. Measurements and Main Results: We performed exome sequencing on an affected sib-pair with normal ultrastructure in more than 85% of cilia. A homozygous splice-site mutation was detected in RSPH1 in both siblings; parents were carriers. Screening RSPH1 in 413 unrelated probands, including 325 with PCD and 88 with idiopathic bronchiectasis, revealed biallelic loss-of-function mutations in nine additional probands. Five affected siblings of probands in RSPH1 families harbored the familial mutations. The 16 individuals with RSPH1 mutations had some features of PCD; however, nasal nitric oxide levels were higher than in patients with PCD with other gene mutations (98.3 vs. 20.7 nl/min; P , 0.0003). Additionally, individuals with RSPH1 mutations had a lower prevalence (8 of 16) of neonatal respiratory distress, and later onset of daily wet cough than typical for PCD, and better lung function (FEV1), compared with 75 age- and sex-matched PCD cases (73.0 vs. 61.8, FEV1 % predicted; P = 0.043). Cilia from individuals with RSPH1 mutations had normal beat frequency (6.16Hz at 258C), but an abnormal, circular beat pattern. Conclusions: The milder clinical disease and higher nasal nitric oxide in individuals with biallelic mutations in RSPH1 provides evidence of a unique genotype-phenotype relationship in PCD, and suggests that mutations in RSPH1 may be associated with residual ciliary function.

Published

2014

49. The Role of Molecular Genetic Analysis in the Diagnosis of Primary Ciliary Dyskinesia

Author

Ernest Cutz, Keith R. Nykamp, Michael R. Knowles, David A. Hall, Maimoona A. Zariwala, Kathleen Nelligan, Raymond H. Kim, and Sharon D. Dell

Subjects

Pulmonary and Respiratory Medicine, Mutation, Pathology, medicine.medical_specialty, animal structures, medicine.diagnostic_test, Genetic disorder, Kartagener Syndrome, Video microscopy, Biology, medicine.disease, medicine.disease_cause, Phenotype, respiratory tract diseases, otorhinolaryngologic diseases, medicine, Motile cilium, Original Research, Genetic testing, Primary ciliary dyskinesia

Abstract

Rationale: Primary ciliary dyskinesia (PCD) is an autosomal recessive genetic disorder of motile cilia. The diagnosis of PCD has previously relied on ciliary analysis with transmission electron microscopy or video microscopy. However, patients with PCD may have normal ultrastructural appearance, and ciliary analysis has limited accessibility. Alternatively, PCD can be diagnosed by demonstrating biallelic mutations in known PCD genes. Genetic testing is emerging as a diagnostic tool to complement ciliary analysis where interpretation and access may delay diagnosis.Objectives: To determine the diagnostic yield of genetic testing of patients with a confirmed or suspected diagnosis of PCD in a multiethnic urban center.Methods: Twenty-eight individuals with confirmed PCD on transmission electron microscopy of ciliary ultrastructure and 24 individuals with a probable diagnosis of PCD based on a classical PCD phenotype and low nasal nitric oxide had molecular analysis of 12 genes associated with PCD.Results: Of ...

Published

2014

50. Mutations in SPAG1 Cause Primary Ciliary Dyskinesia Associated with Defective Outer and Inner Dynein Arms

Author

Whitney E. Wolf, Katrina A. Diaz, Edgar A. Otto, Rim Hjeij, Moumita Chaki, Niki T. Loges, Michael R. Knowles, Petra Pennekamp, Heike Olbrich, Lu Huang, Johanna Raidt, Jan Halbritter, Heon Yung Gee, Heymut Omran, Jay Shendure, Kenneth N. Olivier, Julia Wallmeier, Claudius Werner, Weining Yin, Friedhelm Hildebrandt, Jonathan D. Porath, Michael J. Bamshad, Toby W. Hurd, Matthias Griese, Alexandra P. Lewis, Emily H. Turner, Milan J. Hazucha, Johnny L. Carson, Gerard W. Dougherty, Gyorgy Baktai, Daniela A. Braun, Markus Schueler, Maimoona B Zariwala, Charlotte Jahnke, Thomas W. Ferkol, Sharon D. Dell, Lawrence E. Ostrowski, Margaret W. Leigh, Stephanie D. Davis, Scott D. Sagel, and Deborah A. Nickerson

Subjects

Adult, Male, Cytoplasm, Axoneme, Adolescent, Dynein, Biology, medicine.disease_cause, Young Adult, 03 medical and health sciences, 0302 clinical medicine, GTP-Binding Proteins, Report, otorhinolaryngologic diseases, Genetics, medicine, Animals, Humans, Genetics(clinical), Exome, Cilia, Child, Zebrafish, Genetics (clinical), Exome sequencing, 030304 developmental biology, Primary ciliary dyskinesia, 0303 health sciences, Mutation, Kartagener Syndrome, Cilium, Dyneins, Infant, Epithelial Cells, Inner dynein arm, medicine.disease, Pedigree, Phenotype, Child, Preschool, 030220 oncology & carcinogenesis, Antigens, Surface, Ciliary Motility Disorders, Female

Abstract

Primary ciliary dyskinesia (PCD) is a genetically heterogeneous, autosomal-recessive disorder, characterized by oto-sino-pulmonary disease and situs abnormalities. PCD-causing mutations have been identified in 20 genes, but collectively they account for only ∼65% of all PCDs. To identify mutations in additional genes that cause PCD, we performed exome sequencing on three unrelated probands with ciliary outer and inner dynein arm (ODA+IDA) defects. Mutations in SPAG1 were identified in one family with three affected siblings. Further screening of SPAG1 in 98 unrelated affected individuals (62 with ODA+IDA defects, 35 with ODA defects, 1 without available ciliary ultrastructure) revealed biallelic loss-of-function mutations in 11 additional individuals (including one sib-pair). All 14 affected individuals with SPAG1 mutations had a characteristic PCD phenotype, including 8 with situs abnormalities. Additionally, all individuals with mutations who had defined ciliary ultrastructure had ODA+IDA defects. SPAG1 was present in human airway epithelial cell lysates but was not present in isolated axonemes, and immunofluorescence staining showed an absence of ODA and IDA proteins in cilia from an affected individual, thus indicating that SPAG1 probably plays a role in the cytoplasmic assembly and/or trafficking of the axonemal dynein arms. Zebrafish morpholino studies of spag1 produced cilia-related phenotypes previously reported for PCD-causing mutations in genes encoding cytoplasmic proteins. Together, these results demonstrate that mutations in SPAG1 cause PCD with ciliary ODA+IDA defects and that exome sequencing is useful to identify genetic causes of heterogeneous recessive disorders.

Published

2013