Your search keyword '"Julia Wallmeier"' showing total 39 results

1. Pathogenic KIAA0586/TALPID3 variants are associated with defects in primary and motile cilia

Author

Jacqueline E. Taudien, Diana Bracht, Heike Olbrich, Sebastian Swirski, Fulvio D’Abrusco, Bert Van der Zwaag, Maike Möller, Thomas Lücke, Norbert Teig, Ulrika Lindberg, Kai Wohlgemuth, Julia Wallmeier, Anja Blanque, Christos Gatsogiannis, Sebastian George, Christoph Jüschke, Marta Owczarek-Lipska, Dorothee Veer, Hester Y. Kroes, Enza Maria Valente, G. Christoph Korenke, Heymut Omran, and John Neidhardt

Subjects

Cell biology, Cellular physiology, Human Genetics, Integrative aspects of cell biology, Science

Abstract

Summary: Pathogenic variants in KIAA0586/TALPID3 are associated with the ciliopathy Joubert syndrome (JS). We report individuals with KIAA0586/TALPID3 variants affected by primary and motile cilia defects leading to JS and chronic destructive airway disease. DNA variants were detected in three families by sequencing. In two unrelated families, a deep-intronic variant (KIAA0586/TALPID3:c.3990 + 3186G>A) activated a cryptic exon. We performed histological and functional analyses in native and air-liquid interface (ALI) cultured respiratory cells. Primary cilia lengths were measured in patient-derived fibroblasts. Our data associate KIAA0586/TALPID3 variants with a syndrome combining JS and chronic destructive airway disease, reduced number of motile cilia, disorganized basal body location, and ciliary clearance malfunction. Additionally, patient-derived cell lines showed primary cilia defects. Disease causing KIAA0586/TALPID3 variants, including a deep-intronic sequence variant, were associated with primary and motile cilia defects in JS patients. The combination of JS and respiratory symptoms should be considered indicative for KIAA0586/TALPID3 sequence alterations.

Published

2025

2. CFAP45 deficiency causes situs abnormalities and asthenospermia by disrupting an axonemal adenine nucleotide homeostasis module

Author

Gerard W. Dougherty, Katsutoshi Mizuno, Tabea Nöthe-Menchen, Yayoi Ikawa, Karsten Boldt, Asaf Ta-Shma, Isabella Aprea, Katsura Minegishi, Yuan-Ping Pang, Petra Pennekamp, Niki T. Loges, Johanna Raidt, Rim Hjeij, Julia Wallmeier, Huda Mussaffi, Zeev Perles, Orly Elpeleg, Franziska Rabert, Hidetaka Shiratori, Stef J. Letteboer, Nicola Horn, Samuel Young, Timo Strünker, Friederike Stumme, Claudius Werner, Heike Olbrich, Katsuyoshi Takaoka, Takahiro Ide, Wang Kyaw Twan, Luisa Biebach, Jörg Große-Onnebrink, Judith A. Klinkenbusch, Kavita Praveen, Diana C. Bracht, Inga M. Höben, Katrin Junger, Jana Gützlaff, Sandra Cindrić, Micha Aviram, Thomas Kaiser, Yasin Memari, Petras P. Dzeja, Bernd Dworniczak, Marius Ueffing, Ronald Roepman, Kerstin Bartscherer, Nicholas Katsanis, Erica E. Davis, Israel Amirav, Hiroshi Hamada, and Heymut Omran

Subjects

Science

Abstract

The mechanism by which adenosine monophosphate modulates dynein ATPase-mediated ciliary and flagellar beating remains obscure. Here the authors identify an axonemal module including cilia and flagella associated protein 45 that supports adenine nucleotide homeostasis and underlies a human ciliopathy

Published

2020

3. Collecting clinical data in primary ciliary dyskinesia- challenges and opportunities [version 2; referees: 2 approved]

Author

Israel Amirav, Mary Roduta Roberts, Huda Mussaffi, Avigdor Mandelberg, Yehudah Roth, Revital Abitbul, Anthony Luder, Hannah Blau, Soliman Alkrinawi, Micha Aviram, Marta Ben-Ami, Moshe Rotschild, Lea Bentur, David Shoseyov, Malena Cohen-Cymberknoh, Eitan Kerem, Avraham Avital, Chaim Springer, Avigdor Hevroni, Husein Dabbah, Arnon Elizur, Elie Picard, Shmuel Goldberg, Joseph Rivlin, Galit Livnat, Moran Lavie, Nael Alias, Ruth Soferman, Heike Olbrich, Johanna Raidt, Julia Wallmeier, Claudius Werner, Niki T. Loges, and Heymut Omran

Subjects

Genetics of the Immune System, Methods for Diagnostic & Therapeutic Studies, Medicine, Science

Abstract

Rationale: Primary ciliary dyskinesia (PCD) is under diagnosed and underestimated. Most clinical research has used some form of questionnaires to capture data but none has been critically evaluated particularly with respect to its end-user feasibility and utility. Objective: To critically appraise a clinical data collection questionnaire for PCD used in a large national PCD consortium in order to apply conclusions in future PCD research. Methods: We describe the development, validation and revision process of a clinical questionnaire for PCD and its evaluation during a national clinical PCD study with respect to data collection and analysis, initial completion rates and user feedback. Results: 14 centers participating in the consortium successfully completed the revised version of the questionnaire for 173 patients with various completion rates for various items. While content and internal consistency analysis demonstrated validity, there were methodological deficiencies impacting completion rates and end-user utility. These deficiencies were addressed resulting in a more valid questionnaire. Conclusions: Our experience may be useful for future clinical research in PCD. Based on the feedback collected on the questionnaire through analysis of completion rates, judgmental analysis of the content, and feedback from experts and end users, we suggest a practicable framework for development of similar tools for various future PCD research.

Published

2016

4. Collecting clinical data in primary ciliary dyskinesia- challenges and opportunities [version 1; referees: 2 approved]

Author

Israel Amirav, Mary Roduta Roberts, Huda Mussaffi, Avigdor Mandelberg, Yehudah Roth, Revital Abitbul, Anthony Luder, Hannah Blau, Soliman Alkrinawi, Micha Aviram, Marta Ben-Ami, Moshe Rotschild, Lea Bentur, David Shoseyov, Malena Cohen-Cymberknoh, Eitan Kerem, Avraham Avital, Chaim Springer, Avigdor Hevroni, Husein Dabbah, Arnon Elizur, Elie Picard, Shmuel Goldberg, Joseph Rivlin, Galit Livnat, Moran Lavie, Nael Alias, Ruth Soferman, Heike Olbrich, Johanna Raidt, Julia Wallmeier, Claudius Werner, Niki T. Loges, and Heymut Omran

Subjects

Genetics of the Immune System, Methods for Diagnostic & Therapeutic Studies, Medicine, Science

Abstract

Rationale: Primary ciliary dyskinesia (PCD) is under diagnosed and underestimated. Most clinical research has used some form of questionnaires to capture data but none has been critically evaluated particularly with respect to its end-user feasibility and utility. Objective: To critically appraise a clinical data collection questionnaire for PCD used in a large national PCD consortium in order to apply conclusions in future PCD research. Methods: We describe the development, validation and revision process of a clinical questionnaire for PCD and its evaluation during a national clinical PCD study with respect to data collection and analysis, initial completion rates and user feedback. Results: 14 centers participating in the consortium successfully completed the revised version of the questionnaire for 173 patients with various completion rates for various items. While content and internal consistency analysis demonstrated validity, there were methodological deficiencies impacting completion rates and end-user utility. These deficiencies were addressed resulting in a more valid questionnaire. Conclusions: Our experience may be useful for future clinical research in PCD. Based on the feedback collected on the questionnaire through analysis of completion rates, judgmental analysis of the content, and feedback from experts and end users, we suggest a practicable framework for development of similar tools for various future PCD research.

Published

2016

5. Genetische und diagnostische Charakterisierung einer großen israelischen PCD-Kohorte – Notwendigkeit der geografischen Anpassungen der aktuellen diagnostischen Leitlinien?

Author

Johanna Raidt, Niki T. Loges, Israel Amirav, Sarah Sandmann, Henrike Krenz, Revital Abitbul, Moran Lavie, Huda Mussafi, Avigdor Mandelberg, Alexander Wolter, Gerard W. Dougherty, Tabea Nöthe-Menchen, Julia Wallmeier, Sandra Cindric, Claudius Werner, Petra Pennekamp, Bernd Dworniczak, Miriam Schmidts, Heike Olbrich, Martin Dugas, and Heymut Omran

Published

2023

6. Mutations in TP73 cause impaired mucociliary clearance and lissencephaly

Author

Heike Olbrich, Gerard W. Dougherty, Heymut Omran, Cordula Koerner-Rettberg, Norbert Teig, Christoph M. Heyer, Mohammed Almannai, Eissa Faqeih, Mark Dzietko, Charlotte Thiels, Ibrahim Al Mogarri, Julia Wallmeier, Wadha Al Otaibi, Diana Bracht, Sandra Cindric, Hessa S. Alsaif, Fowzan S. Alkuraya, Sameena Khan, and Aqeela Al-Hashim

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Mucociliary clearance, Medizin, Lissencephaly, Genes, Recessive, Video microscopy, Respiratory Mucosa, Biology, Article, 03 medical and health sciences, 0302 clinical medicine, Loss of Function Mutation, Ciliogenesis, Exome Sequencing, Genetics, medicine, Humans, Basal body, Respiratory system, Cells, Cultured, Genetics (clinical), Primary ciliary dyskinesia, Microscopy, Video, Cilium, Homozygote, Cell Differentiation, Tumor Protein p73, medicine.disease, Ciliopathies, 030104 developmental biology, Mucociliary Clearance, 030217 neurology & neurosurgery

Abstract

Summary TP73 belongs to the TP53 family of transcription factors and has therefore been well studied in cancer research. Studies in mice, however, have revealed non-oncogenic activities related to multiciliogenesis. Utilizing whole-exome sequencing analysis in a cohort of individuals with a mucociliary clearance disorder and cortical malformation, we identified homozygous loss-of-function variants in TP73 in seven individuals from five unrelated families. All affected individuals exhibit a chronic airway disease as well as a brain malformation consistent with lissencephaly. We performed high-speed video microscopy, immunofluorescence analyses, and transmission electron microscopy in respiratory epithelial cells after spheroid or air liquid interface culture to analyze ciliary function, ciliary length, and number of multiciliated cells (MCCs). The respiratory epithelial cells studied display reduced ciliary length and basal bodies mislocalized within the cytoplasm. The number of MCCs is severely reduced, consistent with a reduced number of cells expressing the transcription factors crucial for multiciliogenesis (FOXJ1, RFX2). Our data demonstrate that autosomal-recessive deleterious variants in the TP53 family member TP73 cause a mucociliary clearance disorder due to a defect in MCC differentiation.

Published

2021

7. miR449 Protects Airway Regeneration by Controlling AURKA/HDAC6-Mediated Ciliary Disassembly

Author

Merit Wildung, Christian Herr, Dietmar Riedel, Cornelia Wiedwald, Alena Moiseenko, Fidel Ramírez, Hataitip Tasena, Maren Heimerl, Mihai Alevra, Naira Movsisyan, Maike Schuldt, Larisa Volceanov-Hahn, Sharen Provoost, Tabea Nöthe-Menchen, Diana Urrego, Bernard Freytag, Julia Wallmeier, Christoph Beisswenger, Robert Bals, Maarten van den Berge, Wim Timens, Pieter S. Hiemstra, Corry-Anke Brandsma, Tania Maes, Stefan Andreas, Irene H. Heijink, Luis A. Pardo, Muriel Lizé, Groningen Research Institute for Asthma and COPD (GRIAC), and Guided Treatment in Optimal Selected Cancer Patients (GUTS)

Subjects

CDC20B, miR449, Histone Deacetylase 6, Catalysis, Aurora Kinase A/genetics, lung, Pulmonary Disease, Inorganic Chemistry, Pulmonary Disease, Chronic Obstructive, Mice, Cilia/genetics, Tubulin, Chronic Obstructive/genetics, Medicine and Health Sciences, Animals, COPD, Cilia, Physical and Theoretical Chemistry, Molecular Biology, Spectroscopy, Aurora Kinase A, microRNA, Organic Chemistry, Epithelial Cells, General Medicine, ciliogenesis, airway, miR449a, Pulmonary Disease, Chronic Obstructive/genetics, Computer Science Applications, MicroRNAs, MicroRNAs/genetics, Tubulin/genetics

Abstract

Airway mucociliary regeneration and function are key players for airway defense and are impaired in chronic obstructive pulmonary disease (COPD). Using transcriptome analysis in COPD-derived bronchial biopsies, we observed a positive correlation between cilia-related genes and microRNA-449 (miR449). In vitro, miR449 was strongly increased during airway epithelial mucociliary differentiation. In vivo, miR449 was upregulated during recovery from chemical or infective insults. miR0449−/− mice (both alleles are deleted) showed impaired ciliated epithelial regeneration after naphthalene and Haemophilus influenzae exposure, accompanied by more intense inflammation and emphysematous manifestations of COPD. The latter occurred spontaneously in aged miR449−/− mice. We identified Aurora kinase A and its effector target HDAC6 as key mediators in miR449-regulated ciliary homeostasis and epithelial regeneration. Aurora kinase A is downregulated upon miR449 overexpression in vitro and upregulated in miR449−/− mouse lungs. Accordingly, imaging studies showed profoundly altered cilia length and morphology accompanied by reduced mucociliary clearance. Pharmacological inhibition of HDAC6 rescued cilia length and coverage in miR449−/− cells, consistent with its tubulin-deacetylating function. Altogether, our study establishes a link between miR449, ciliary dysfunction, and COPD pathogenesis.

Published

2022

8. Loss of CBY1 results in a ciliopathy characterized by features of Joubert syndrome

Author

Dan Doherty, Nadine Bachmann, Rachel H. Giles, Erica E. Davis, Asbjørn Holmgren, Dulika S. Sumathipala, Barbara Käsmann-Kellner, Lokuliyange D S Senaratne, Suzanne Crowley, Sebastian Patzke, Nicholas Katsanis, Petter Strømme, Daniel Epting, Christian Decker, Kari-Anne M Frikstad, Carsten Bergmann, Manuela Zucknick, Diana Bracht, Tuva Barøy, Elisabeth Ott, Eva Decker, Soeren S. Lienkamp, Doriana Misceo, Ian G. Phelps, Heymut Omran, Miriam Schmidts, Alma Sikiric, Selma Mujezinovic Larsen, Julia Wallmeier, and Eirik Frengen

Subjects

Male, Pathology, Ciliopathies, whole exome sequencing, CBY1, Cerebellum, Eye Abnormalities, Child, Research Articles, Zebrafish, Genetics (clinical), Exome sequencing, 0303 health sciences, Polydactyly, Cilium, Homozygote, 030305 genetics & heredity, Nuclear Proteins, Kidney Diseases, Cystic, Magnetic Resonance Imaging, Smoothened Receptor, Pedigree, 3. Good health, Phenotype, Child, Preschool, primary cilia defect, Female, medicine.symptom, Research Article, medicine.medical_specialty, Adolescent, Biology, Retina, Joubert syndrome, Young Adult, 03 medical and health sciences, Genetics, medicine, Animals, Humans, Abnormalities, Multiple, Cilia, 030304 developmental biology, Cerebellar ataxia, Genetic heterogeneity, Infant, Newborn, Infant, Fibroblasts, medicine.disease, Ciliopathy, ciliopathy, Mutation, Carrier Proteins

Abstract

Ciliopathies are clinically and genetically heterogeneous diseases. We studied three patients from two independent families presenting with features of Joubert syndrome: abnormal breathing pattern during infancy, developmental delay/intellectual disability, cerebellar ataxia, molar tooth sign on magnetic resonance imaging scans, and polydactyly. We identified biallelic loss‐of‐function (LOF) variants in CBY1, segregating with the clinical features of Joubert syndrome in the families. CBY1 localizes to the distal end of the mother centriole, contributing to the formation and function of cilia. In accordance with the clinical and mutational findings in the affected individuals, we demonstrated that depletion of Cby1 in zebrafish causes ciliopathy‐related phenotypes. Levels of CBY1 transcript were found reduced in the patients compared with controls, suggesting degradation of the mutated transcript through nonsense‐mediated messenger RNA decay. Accordingly, we could detect CBY1 protein in fibroblasts from controls, but not from patients by immunofluorescence. Furthermore, we observed reduced ability to ciliate, increased ciliary length, and reduced levels of the ciliary proteins AHI1 and ARL13B in patient fibroblasts. Our data show that CBY1 LOF‐variants cause a ciliopathy with features of Joubert syndrome.

Published

2020

9. The role of cilia for hydrocephalus formation

Author

Julia Wallmeier, Marlene Dallmayer, and Heymut Omran

Subjects

Genetics, Infant, Newborn, Humans, Cilia, Nervous System Malformations, Genetics (clinical), Ciliopathies, Hydrocephalus

Abstract

Hydrocephalus is a common finding in newborns. In most cases, it is caused by intraventricular hemorrhage associated with prematurity, whereas in some patients the cause of hydrocephalus can be traced back to genetic changes, associated with disease syndromes such as RASopathies, lysosomal storage diseases, dystroglycanopathies, craniosynostosis but also ciliopathies. Ciliopathies are a group of diseases that can affect multiple organ systems due to dysfunction or the absence of cilia. Cilia are small organelles, extending from the cell surface. Nonmotile monocilia are ubiquitously present during cell development fulfilling chemosensory functions, whereas specialized epithelia such as the ependyma, lining the inner surface of the brain ventricles, exhibit multiciliated cells propelling fluids along the cell surface. This review highlights ciliopathies and their pathophysiology in congenital hydrocephalus. While nonmotile ciliopathies are often associated with severe prenatal hydrocephalus combined with other severe congenital brain malformations, motile ciliopathies, especially those associated with defects in multiciliogenesis can cause hydrocephalus and chronic lung disease.

Published

2022

10. Limitations of Nasal Nitric Oxide Measurement for Diagnosis of Primary Ciliary Dyskinesia with Normal Ultrastructure

Author

Johanna Raidt, Henrike Krenz, Johannes Tebbe, Jörg Große-Onnebrink, Heike Olbrich, Niki Tomas Loges, Luisa Biebach, Christian Schmalstieg, Christina Keßler, Julia Wallmeier, Bernd Dworniczak, Petra Pennekamp, Martin Dugas, Claudius Werner, and Heymut Omran

Subjects

Pulmonary and Respiratory Medicine, Cohort Studies, Phenotype, Kartagener Syndrome, Humans, Cilia, Nitric Oxide, Ciliary Motility Disorders

Published

2022

11. Mutations in TP73 Cause Cortical Malformation Consistent with Lissencephaly

Author

Christoph M. Heyer, Heike Olbrich, Mark Dzietko, Charlotte Thiels, Hessa S. Alsaif, Fowzan S. Alkuraya, Cordula Koerner-Rettberg, Heymut Omran, Norbert Teig, Julia Wallmeier, Gerard W. Dougherty, Diana Bracht, and Sandra Cindric

Subjects

Pathology, medicine.medical_specialty, business.industry, medicine, Lissencephaly, medicine.disease, business

Published

2021

12. Diagnosis of Primary Ciliary Dyskinesia: a multi-center experience

Author

Heike Olbrich, Julia Wallmeier, Heymut Omran, Petra Pennekamp, Niki T. Loges, Gerard W. Dougherty, Johanna Raidt, Rim Hjeij, and Sandra Cindric

Subjects

medicine.medical_specialty, business.industry, Ophthalmology, medicine, Center (algebra and category theory), medicine.disease, business, Primary ciliary dyskinesia

Published

2021

13. 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

14. Motility of efferent duct cilia aids passage of sperm cells through the male reproductive system

Author

Tabea Nöthe-Menchen, Heymut Omran, Gerard W. Dougherty, Julia Wallmeier, Thomas Kaiser, Timo Strünker, Petra Pennekamp, Heike Olbrich, Isabella Aprea, Sabine Kliesch, Niki T. Loges, and Johanna Raidt

Subjects

0301 basic medicine, Male, Embryology, Axoneme, Mice, 129 Strain, Movement, Mice, Transgenic, Biology, Genitalia, Male, Asthenozoospermia, efferent ducts / cilia / sperm / motor proteins / outer dynein arm-defects / DNAH5 / 45 male infertility / oligozoospermia / motile ciliopathy / primary ciliary dyskinesia, Andrology, 03 medical and health sciences, 0302 clinical medicine, Genetics, medicine, Animals, Humans, Genetic Predisposition to Disease, Cilia, Molecular Biology, Sperm motility, Primary ciliary dyskinesia, Original Research, 030219 obstetrics & reproductive medicine, Obstetrics and Gynecology, Efferent ducts, Cell Biology, Axonemal Dyneins, Oligospermia, medicine.disease, Epididymis, Sperm, Spermatozoa, AcademicSubjects/MED00905, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Phenotype, Reproductive Medicine, Mutation, Motile cilium, Sperm Motility, Outer dynein arm, Developmental Biology, Ciliary Motility Disorders

Abstract

Motile cilia line the efferent ducts of the mammalian male reproductive tract. Several recent mouse studies have demonstrated that a reduced generation of multiple motile cilia in efferent ducts is associated with obstructive oligozoospermia and fertility issues. However, the sole impact of efferent duct cilia dysmotility on male infertility has not been studied so far either in mice or human. Using video microscopy, histological- and ultrastructural analyses, we examined male reproductive tracts of mice deficient for the axonemal motor protein DNAH5: this defect exclusively disrupts the outer dynein arm (ODA) composition of motile cilia but not the ODA composition and motility of sperm flagella. These mice have immotile efferent duct cilia that lack ODAs, which are essential for ciliary beat generation. Furthermore, they show accumulation of sperm in the efferent duct. Notably, the ultrastructure and motility of sperm from these males are unaffected. Likewise, human individuals with loss-of-function DNAH5 mutations present with reduced sperm count in the ejaculate (oligozoospermia) and dilatations of the epididymal head but normal sperm motility, similar to DNAH5 deficient mice. The findings of this translational study demonstrate, in both mice and men, that efferent duct ciliary motility is important for male reproductive fitness and uncovers a novel pathomechanism distinct from primary defects of sperm motility (asthenozoospermia). If future work can identify environmental factors or defects in genes other than DNAH5 that cause efferent duct cilia dysmotility, this will help unravel other causes of oligozoospermia and may influence future practices in genetic and fertility counseling as well as ART.

Published

2020

15. Mutation of serine/threonine protein kinase 36 ( STK36 ) causes primary ciliary dyskinesia with a central pair defect

Author

Gerard W. Dougherty, Heike Olbrich, Christine Edelbusch, Niki T. Loges, Joseph Rivlin, Heymut Omran, Petra Pennekamp, Julia Wallmeier, Sandra Cindric, and Israel Amirav

Subjects

Male, 0301 basic medicine, Pathology, medicine.medical_specialty, Axoneme, Respiratory Mucosa, Serine threonine protein kinase, Protein Serine-Threonine Kinases, Biology, medicine.disease_cause, Cell Line, 03 medical and health sciences, 0302 clinical medicine, Radial spoke, otorhinolaryngologic diseases, Genetics, medicine, Humans, Genetics (clinical), Primary ciliary dyskinesia, Mutation, Cilium, Dyneins, Kartagener Syndrome, Epithelial Cells, Anatomy, medicine.disease, respiratory tract diseases, Situs inversus, Phenotype, 030104 developmental biology, medicine.anatomical_structure, Female, Situs solitus, 030217 neurology & neurosurgery, Ciliary Motility Disorders

Abstract

Primary ciliary dyskinesia (PCD) is a genetic condition of impaired ciliary beating, characterized by chronic infections of the upper and lower airways and progressive lung failure. Defects of the outer dynein arms are the most common cause of PCD. In about half of the affected individuals, PCD occurs with situs inversus (Kartagener syndrome). A minor PCD subgroup including defects of the radial spokes (RS) and central pair (CP) is hallmarked by the absence of laterality defects, subtle beating abnormalities, and unequivocally apparent ultrastructural defects of the ciliary axoneme, making their diagnosis challenging. We identified homozygous loss-of-function mutations in STK36 in one PCD-affected individual with situs solitus. Transmission electron microscopy analysis demonstrates that STK36 is required for cilia orientation in human respiratory epithelial cells, with a probable localization of STK36 between the RS and CP. STK36 screening can now be included for this rare and difficult to diagnose PCD subgroup.

Published

2017

16. CFAP45 deficiency causes situs abnormalities and asthenospermia by disrupting an axonemal adenine nucleotide homeostasis module

Author

Hidetaka Shiratori, Claudius Werner, Kavita Praveen, Stef J.F. Letteboer, Petra Pennekamp, Petras P. Dzeja, Katrin Junger, Inga M. Höben, Franziska Rabert, Friederike Stumme, Julia Wallmeier, Isabella Aprea, Zeev Perles, Erica E. Davis, Judith A. Klinkenbusch, Israel Amirav, Yasin Memari, Yayoi Ikawa, Niki T. Loges, Diana Bracht, Wang Kyaw Twan, Kerstin Bartscherer, Tabea Nöthe-Menchen, Micha Aviram, Yuan Ping Pang, Rim Hjeij, Johanna Raidt, Heike Olbrich, Huda Mussaffi, Katsutoshi Mizuno, Nicola Horn, Timo Strünker, Heymut Omran, Sandra Cindric, Asaf Ta-Shma, Gerard W. Dougherty, Katsuyoshi Takaoka, Marius Ueffing, Thomas Kaiser, Katsura Minegishi, Jörg Große-Onnebrink, Hiroshi Hamada, Jana Gützlaff, Bernd Dworniczak, Luisa Biebach, Samuel M. Young, Orly Elpeleg, Nicholas Katsanis, Karsten Boldt, Takahiro Ide, Ronald Roepman, and Hubrecht Institute for Developmental Biology and Stem Cell Research

Subjects

0301 basic medicine, Male, Axoneme, DNA Mutational Analysis, General Physics and Astronomy, Diseases, Whole Exome Sequencing, chemistry.chemical_compound, Mice, 0302 clinical medicine, Cilia/metabolism, Adenine nucleotide, Loss of Function Mutation, Epididymis/pathology, Sperm Motility/genetics, Axoneme/ultrastructure, lcsh:Science, Tomography, Epididymis, Mice, Knockout, Multidisciplinary, Adenine Nucleotides, Adenine Nucleotides/metabolism, Cilium, CRISPR-Cas Systems/genetics, Microtubule sliding, Middle Aged, Situs Inversus, Respiratory Mucosa/cytology, Cell biology, X-Ray Computed, Asthenozoospermia, Flagella, Sperm Motility, Female, Adenosine monophosphate, Adult, Adolescent, Science, Knockout, Dynein, Adenylate kinase, Respiratory Mucosa, General Biochemistry, Genetics and Molecular Biology, Article, Asthenozoospermia/genetics, 03 medical and health sciences, Exome Sequencing, Planarians/cytology, Genetics, Animals, Humans, Cilia, Cytoskeletal Proteins/deficiency, Situs Inversus/diagnostic imaging, Flagella/metabolism, Animal, General Chemistry, Planarians, Adenosine diphosphate, Cytoskeletal Proteins, Disease Models, Animal, 030104 developmental biology, Renal disorders Radboud Institute for Molecular Life Sciences [Radboudumc 11], chemistry, Disease Models, lcsh:Q, CRISPR-Cas Systems, Tomography, X-Ray Computed, Adenosine triphosphate, 030217 neurology & neurosurgery

Abstract

Axonemal dynein ATPases direct ciliary and flagellar beating via adenosine triphosphate (ATP) hydrolysis. The modulatory effect of adenosine monophosphate (AMP) and adenosine diphosphate (ADP) on flagellar beating is not fully understood. Here, we describe a deficiency of cilia and flagella associated protein 45 (CFAP45) in humans and mice that presents a motile ciliopathy featuring situs inversus totalis and asthenospermia. CFAP45-deficient cilia and flagella show normal morphology and axonemal ultrastructure. Proteomic profiling links CFAP45 to an axonemal module including dynein ATPases and adenylate kinase as well as CFAP52, whose mutations cause a similar ciliopathy. CFAP45 binds AMP in vitro, consistent with structural modelling that identifies an AMP-binding interface between CFAP45 and AK8. Microtubule sliding of dyskinetic sperm from Cfap45−/− mice is rescued with the addition of either AMP or ADP with ATP, compared to ATP alone. We propose that CFAP45 supports mammalian ciliary and flagellar beating via an adenine nucleotide homeostasis module., The mechanism by which adenosine monophosphate modulates dynein ATPase-mediated ciliary and flagellar beating remains obscure. Here the authors identify an axonemal module including cilia and flagella associated protein 45 that supports adenine nucleotide homeostasis and underlies a human ciliopathy

Published

2020

17. Randomization of Left-Right Asymmetry and Congenital Heart Defects

Author

Bernd Dworniczak, Tabea Nöthe-Menchen, Petra Pennekamp, Johanna Raidt, Heymut Omran, Inga M. Höben, Heike Olbrich, Julia Wallmeier, Rim Hjeij, Niki T. Loges, Gerard W. Dougherty, and University of Zurich

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, business.industry, Cilium, Nodal signaling, Situs ambiguus, 610 Medicine & health, General Medicine, 030204 cardiovascular system & hematology, medicine.disease, Phenotype, 03 medical and health sciences, Situs inversus, 030104 developmental biology, 0302 clinical medicine, 10036 Medical Clinic, Laterality, otorhinolaryngologic diseases, Motile cilium, medicine, business, Primary ciliary dyskinesia

Abstract

Background: Nearly one in 100 live births presents with congenital heart defects (CHD). CHD is frequently associated with laterality defects, such as situs inversus , a mirrored positioning of internal organs. Body laterality is established by a complex process: monocilia at the embryonic left-right organizer facilitate both the generation and sensing of a leftward fluid flow. This induces the conserved left-sided Nodal signaling cascade to initiate asymmetrical organogenesis. Primary ciliary dyskinesia originates from dysfunction of motile cilia, causing symptoms such as chronic sinusitis, bronchiectasis and frequently situs inversus totalis . The most frequently mutated gene in primary ciliary dyskinesia, DNAH5 is associated with randomization of body asymmetry resulting in situs inversus totalis in half of the patients; however, its relation to CHD occurrence in humans has not been investigated in detail so far. Methods: We performed genotype/phenotype correlations in 132 patients with primary ciliary dyskinesia carrying disease-causing DNAH5 mutations, focusing on situs defects and CHD. Using high-speed video microscopy-, immunofluorescence-, and in situ hybridization analyses, we investigated the initial steps of left-right axis establishment in embryos of a Dnah5 -mutant mouse model. Results: In patients with primary ciliary dyskinesia carrying disease-causing DNAH5 mutations, 65.9% (87/132) had laterality defects: 88.5% (77/87) presented with situs inversus totalis , 11.5% (10/87) presented with situs ambiguus ; and 6.1% (8/132) presented with CHD. In Dnah5 mut/mut mice, embryonic left-right organizer monocilia lack outer dynein arms resulting in immotile cilia, impaired flow at the left-right organizer, and randomization of Nodal signaling with normal, reversed or bilateral expression of key molecules. Conclusions: For the first time, we directly demonstrate the disease-mechanism of laterality defects linked to DNAH5 deficiency at the molecular level during embryogenesis. We highlight that mutations in DNAH5 are not only associated with classical randomization of left-right body asymmetry but also with severe laterality defects including CHD.

Published

2019

18. Randomization of Left-right Asymmetry and Congenital Heart Defects: The Role of

Author

Tabea, Nöthe-Menchen, Julia, Wallmeier, Petra, Pennekamp, Inga M, Höben, Heike, Olbrich, Niki T, Loges, Johanna, Raidt, Gerard W, Dougherty, Rim, Hjeij, Bernd, Dworniczak, and Heymut, Omran

Subjects

Article

Abstract

BACKGROUND: Nearly one in 100 live births presents with congenital heart defects (CHD). CHD are frequently associated with laterality defects, such as situs inversus totalis (SIT), a mirrored positioning of internal organs. Body laterality is established by a complex process: monocilia at the embryonic left-right organizer (LRO) facilitate both the generation and sensing of a leftward fluid flow. This induces the conserved left-sided Nodal signaling cascade to initiate asymmetric organogenesis. Primary ciliary dyskinesia (PCD) originates from dysfunction of motile cilia, causing symptoms such as chronic sinusitis, bronchiectasis and frequently SIT. The most frequently mutated gene in PCD, DNAH5 is associated with randomization of body asymmetry resulting in SIT in half of the patients; however, its relation to CHD occurrence in humans has not been investigated in detail so far. METHODS: We performed genotype / phenotype correlations in 132 PCD patients carrying disease-causing DNAH5 mutations, focusing on situs defects and CHD. Using high speed video microscopy-, immunofluorescence-, and in situ hybridization analyses, we investigated the initial steps of left-right axis establishment in embryos of a Dnah5 mutant mouse model. RESULTS: 65.9% (87 / 132) of the PCD patients carrying disease-causing DNAH5 mutations had laterality defects: 88.5% (77 / 87) presented with SIT, 11.5% (10 / 87) presented with situs ambiguus; and 6.1% (8 / 132) presented with CHD. In Dnah5(mut/mut) mice, embryonic LRO monocilia lack outer dynein arms resulting in immotile cilia, impaired flow at the LRO, and randomization of Nodal signaling with normal, reversed or bilateral expression of key molecules. CONCLUSIONS: For the first time, we directly demonstrate the disease-mechanism of laterality defects linked to DNAH5 deficiency at the molecular level during embryogenesis. We highlight that mutations in DNAH5 are not only associated with classical randomization of left-right body asymmetry but also with severe laterality defects including CHD.

Published

2019

19. 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

20. Primary ciliary dyskinesia in Israel: Prevalence, clinical features, current diagnosis and management practices

Author

Ruth Soferman, Soliman Alkrinawi, Elie Picard, Lea Bentur, Shmuel Goldberg, Chaim Springer, Joseph Rivlin, Avigdor Mandelberg, Anthony Luder, Moshe Rotschild, Arnon Elizur, Eitan Kerem, Yehudah Roth, Julia Wallmeier, Husein Dabbah, Martina Herting, Micha Aviram, Hannah Blau, David Shoseyov, Claudius Werner, Heymut Omran, Nael Elias, Malena Cohen-Cymberknoh, Israel Amirav, Alexander Wolter, Johanna Raidt, Marta Ben Ami, Avigdor Hevroni, Avraham Avital, Dario Prais, Galit Livnat, Moran Lavie, Niki T. Loges, Revital Abitbul, Huda Mussaffi, and Heike Olbrich

Subjects

Adult, Male, 0301 basic medicine, Pulmonary and Respiratory Medicine, Neonatal pneumonia, Pediatrics, medicine.medical_specialty, Adolescent, Referral, Population, Nitric Oxide, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Microscopy, Electron, Transmission, Prevalence, otorhinolaryngologic diseases, medicine, Humans, Cilia, Prospective Studies, Israel, Child, education, Management practices, Primary ciliary dyskinesia, education.field_of_study, Bronchiectasis, Kartagener Syndrome, business.industry, medicine.disease, Situs inversus, 030104 developmental biology, 030228 respiratory system, Multicenter study, Female, business

Abstract

Primary Ciliary Dyskinesia (PCD) is rare and its features in Israel have not been described.to assess prevalence utilizing state-of-the-art diagnostic techniques, and describe clinical features, diagnostic and management practices in Israel.A national multicenter study from 2012 to 2013 recruited patients diagnosed or suspected of having PCD. Diagnosis was verified using: nasal Nitric Oxide (nNO); High-speed Video Microscope Analysis (HVMA); Transmission Electron Microscopy (TEM) of cilia; Immuno-fluorescence staining (IF) for ciliary proteins, and genetic analysis.Of the 203 patients recruited from 14 pediatric centers, 150 had a PCD diagnosis verified. Median age was 15.05y, with range 0.15-60.5y. PCD prevalence was 1:54,000 for the general population and 1:25,000 in children (5-14 y). For the non-Jewish (mainly Druze and Arab Moslem) compared to Jewish populations, prevalence was 1:16,500 and 1:139,000 respectively (p 0.0001) and parental consanguinity was 85.4% and 21.9% respectively (p 0.0001). Clinical features included bronchiectasis (88%), rhinitis (81%), recurrent pneumonia (78%), recurrent otitis (62%), neonatal pneumonia (60%) and situs inversus (42%). Prior diagnostic practices varied widely between centers with TEM assessed in 55% and abnormal in 61% of these. Management included antibiotics and airway clearance. Diagnostic verification revealed for 150 PCD patients: 81% nNO233 ppb, 62% abnormal HVMA, 51% diagnostic TEM, 58% diagnostic IF and, 57% genetic diagnosis.PCD in Israel is rare, with comprehensive diagnostic tests showing prevalence in children similar to Europe. Prevalence was higher in non-Jews, associated with parental consanguinity. Diagnostic and management practices vary. Referral centers providing comprehensive diagnostic and care capabilities should be established.

Published

2016

21. DNAH11 Localization in the Proximal Region of Respiratory Cilia Defines Distinct Outer Dynein Arm Complexes

Author

Artem Shaposhnykov, Gerard W. Dougherty, Lea Bentur, Virginia Mirra, Julia Wallmeier, Martina Brueckner, Kavita Praveen, Heike Olbrich, Sara Kashef, Yasin Memari, Pekka Valmari, Heymut Omran, Claudius Werner, Mohammad Amin Kashef, Erica E. Davis, Bernd Dworniczak, Niki T. Loges, Christian Ruckert, Karsten Häffner, Johanna Raidt, Nicholas Katsanis, Micha Aviram, Gaia Pigino, Israel Amirav, Cordula Westermann, Anja Kolb-Kokocinski, Gyorgy Baktai, Tabea Menchen, Fardin Eghtedari, Judith A. Klinkenbusch, Rim Hjeij, Petra Pennekamp, and Richard Durbin

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, Mucociliary clearance, Clinical Biochemistry, Dynein, Context (language use), Biology, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Cilia, Lung, Molecular Biology, Original Research, Primary ciliary dyskinesia, Base Sequence, Kartagener Syndrome, Cilium, Homozygote, Dyneins, Axonemal Dyneins, Cell Biology, medicine.disease, Cell biology, Protein Transport, 030104 developmental biology, medicine.anatomical_structure, 030228 respiratory system, Mutation, Outer dynein arm

Abstract

Primary ciliary dyskinesia (PCD) is a recessively inherited disease that leads to chronic respiratory disorders owing to impaired mucociliary clearance. Conventional transmission electron microscopy (TEM) is a diagnostic standard to identify ultrastructural defects in respiratory cilia but is not useful in approximately 30% of PCD cases, which have normal ciliary ultrastructure. DNAH11 mutations are a common cause of PCD with normal ciliary ultrastructure and hyperkinetic ciliary beating, but its pathophysiology remains poorly understood. We therefore characterized DNAH11 in human respiratory cilia by immunofluorescence microscopy (IFM) in the context of PCD. We used whole-exome and targeted next-generation sequence analysis as well as Sanger sequencing to identify and confirm eight novel loss-of-function DNAH11 mutations. We designed and validated a monoclonal antibody specific to DNAH11 and performed high-resolution IFM of both control and PCD-affected human respiratory cells, as well as samples from green fluorescent protein (GFP)-left-right dynein mice, to determine the ciliary localization of DNAH11. IFM analysis demonstrated native DNAH11 localization in only the proximal region of wild-type human respiratory cilia and loss of DNAH11 in individuals with PCD with certain loss-of-function DNAH11 mutations. GFP-left-right dynein mice confirmed proximal DNAH11 localization in tracheal cilia. DNAH11 retained proximal localization in respiratory cilia of individuals with PCD with distinct ultrastructural defects, such as the absence of outer dynein arms (ODAs). TEM tomography detected a partial reduction of ODAs in DNAH11-deficient cilia. DNAH11 mutations result in a subtle ODA defect in only the proximal region of respiratory cilia, which is detectable by IFM and TEM tomography.

Published

2016

22. TTC25 Deficiency Results in Defects of the Outer Dynein Arm Docking Machinery and Primary Ciliary Dyskinesia with Left-Right Body Asymmetry Randomization

Author

Heymut Omran, Gerard W. Dougherty, Julia Wallmeier, John B. Wallingford, Heike Olbrich, Yasuko Asai, Chanjae Lee, Sascha Sauer, Yasin Memari, Kyosuke Shinohara, Petra Pennekamp, Matthias Griese, Johanna Raidt, Anja Kolb-Kokocinski, Tabea Menchen, Hidetaka Shiratori, Rim Hjeij, Christine Edelbusch, Richard Durbin, Claudius Werner, Hiroshi Hamada, Katsura Minegishi, Niki T. Loges, and Katsuyoshi Takaoka

Subjects

0301 basic medicine, Axoneme, Xenopus, Dynein, Fluorescent Antibody Technique, Genes, Recessive, Biology, Xenopus Proteins, 03 medical and health sciences, Mice, 0302 clinical medicine, Microscopy, Electron, Transmission, Report, medicine, Genetics, Animals, Humans, Exome, Genetics(clinical), Cilia, Genetics (clinical), Primary ciliary dyskinesia, Kartagener Syndrome, Cilium, Dyneins, Anatomy, Exons, medicine.disease, biology.organism_classification, Cell biology, 030104 developmental biology, 030220 oncology & carcinogenesis, Mutation, Outer dynein arm, NODAL, Carrier Proteins, Congenital disorder, Protein Binding

Abstract

Multiprotein complexes referred to as outer dynein arms (ODAs) develop the main mechanical force to generate the ciliary and flagellar beat. ODA defects are the most common cause of primary ciliary dyskinesia (PCD), a congenital disorder of ciliary beating, characterized by recurrent infections of the upper and lower airways, as well as by progressive lung failure and randomization of left-right body asymmetry. Using a whole-exome sequencing approach, we identified recessive loss-of-function mutations within TTC25 in three individuals from two unrelated families affected by PCD. Mice generated by CRISPR/Cas9 technology and carrying a deletion of exons 2 and 3 in Ttc25 presented with laterality defects. Consistently, we observed immotile nodal cilia and missing leftward flow via particle image velocimetry. Furthermore, transmission electron microscopy (TEM) analysis in TTC25-deficient mice revealed an absence of ODAs. Consistent with our findings in mice, we were able to show loss of the ciliary ODAs in humans via TEM and immunofluorescence (IF) analyses. Additionally, IF analyses revealed an absence of the ODA docking complex (ODA-DC), along with its known components CCDC114, CCDC151, and ARMC4. Co-immunoprecipitation revealed interaction between the ODA-DC component CCDC114 and TTC25. Thus, here we report TTC25 as a new member of the ODA-DC machinery in humans and mice.

Published

2016

23. FV 1177. Genetic Causes of Congenital Hydrocephalus

Author

Heymut Omran, Angela Brentrup, Julia Wallmeier, Barbara Fiedler, Diana Frank, and Oliver Schwarz

Subjects

Pediatrics, medicine.medical_specialty, business.industry, Medicine, business, Congenital hydrocephalus

Published

2018

24. Systematic Analysis ofCCNOVariants in a Defined Population: Implications for Clinical Phenotype and Differential Diagnosis

Author

Israel, Amirav, Julia, Wallmeier, Niki T, Loges, Tabea, Menchen, Petra, Pennekamp, Huda, Mussaffi, Revital, Abitbul, Avraham, Avital, Lea, Bentur, Gerard W, Dougherty, Elias, Nael, Moran, Lavie, Heike, Olbrich, Claudius, Werner, Chris, Kintner, Heymut, Omran, and Ruth, Soferman

Subjects

Male, 0301 basic medicine, Mucociliary clearance, DNA Mutational Analysis, Population, Mutation, Missense, Biology, medicine.disease_cause, DNA Glycosylases, Diagnosis, Differential, Mice, Xenopus laevis, 03 medical and health sciences, 0302 clinical medicine, Genetics, medicine, Animals, Humans, Missense mutation, Genetic Testing, Frameshift Mutation, education, Genetic Association Studies, Genetics (clinical), Primary ciliary dyskinesia, education.field_of_study, Mutation, Genetic Variation, medicine.disease, Phenotype, Respiratory Function Tests, Protein Transport, 030104 developmental biology, Genetic Loci, 030220 oncology & carcinogenesis, Immunology, Motile cilium, Ciliary Motility Disorders, Female, Radiography, Thoracic, Tomography, X-Ray Computed

Abstract

Reduced generation of multiple motile cilia (RGMC) is a novel chronic destructive airway disease within the group of mucociliary clearance disorders with only few cases reported. Mutations in two genes, CCNO and MCIDAS, have been identified as a cause of this disease, both leading to a greatly reduced number of cilia and causing impaired mucociliary clearance. This study was designed to identify the prevalence of CCNO mutations in Israel and further delineate the clinical characteristics of RGMC. We analyzed 170 families with mucociliary clearance disorders originating from Israel for mutations in CCNO and identified two novel mutations (c.165delC, p.Gly56Alafs*38; c.638T>C, p.Leu213Pro) and two known mutations in 15 individuals from 10 families (6% prevalence). Pathogenicity of the missense mutation (c.638T>C, p.Leu213Pro) was demonstrated by functional analyses in Xenopus. Combining these 15 patients with the previously reported CCNO case reports revealed rapid deterioration in lung function, an increased prevalence of hydrocephalus (10%) as well as increased female infertility (22%). Consistent with these findings, we demonstrate that CCNO expression is present in murine ependyma and fallopian tubes. CCNO is mutated more frequently than expected from the rare previous clinical case reports, leads to severe clinical manifestations, and should therefore be considered an important differential diagnosis of mucociliary clearance disorders.

Published

2016

25. Mutations in C11orf70 Cause Primary Ciliary Dyskinesia with Randomization of Left/Right Body Asymmetry Due to Defects of Outer and Inner Dynein Arms

Author

Gerard W. Dougherty, Petra Pennekamp, Johanna Raidt, Inga M. Höben, Laura Venditto, Julia Wallmeier, Israel Amirav, Tabea Nöthe-Menchen, Heymut Omran, Diana Frank, Huda Mussaffi, Kaman Wu, Kim G. Nielsen, Niki T. Loges, Maria C. Philipsen, Bernd Dworniczak, Zeineb Bakey, Isabella Aprea, Francesca Santamaria, Miriam Schmidts, Freerk Prenzel, Rim Hjeij, Heike Olbrich, Höben, Inga M., Hjeij, Rim, Olbrich, Heike, Dougherty, Gerard W., Nöthe-Menchen, Tabea, Aprea, Isabella, Frank, Diana, Pennekamp, Petra, Dworniczak, Bernd, Wallmeier, Julia, Raidt, Johanna, Nielsen, Kim G., Philipsen, Maria C., Santamaria, Francesca, Venditto, Laura, Amirav, Israel, Mussaffi, Huda, Prenzel, Freerk, Wu, Kaman, Bakey, Zeineb, Schmidts, Miriam, Loges, Niki T., and Omran, Heymut

Subjects

Male, 0301 basic medicine, primary ciliary dyskinesia, Genes, Recessive, Flagellum, Biology, Male infertility, Pathogenesis, 03 medical and health sciences, All institutes and research themes of the Radboud University Medical Center, dynein arm, Genetic, Loss of Function Mutation, Report, Ciliogenesis, preassembly, Genetics, medicine, Humans, Genetics (clinical), Nuclear Protein, Body Patterning, Primary ciliary dyskinesia, Kartagener Syndrome, Cilium, cilia, Dynein, Dyneins, Nuclear Proteins, C11ORF70, medicine.disease, Sperm, sperm flagella, 3. Good health, Cell biology, Renal disorders Radboud Institute for Molecular Life Sciences [Radboudumc 11], 030104 developmental biology, Sperm Tail, Mutation, Motile cilium, Female, Human

Abstract

Primary ciliary dyskinesia (PCD) is characterized by chronic airway disease, male infertility, and randomization of the left/right body axis as a result of defects of motile cilia and sperm flagella. We identified loss-of-function mutations in the open-reading frame C11orf70 in PCD individuals from five distinct families. Transmission electron microscopy analyses and high-resolution immunofluorescence microscopy demonstrate that loss-of-function mutations in C11orf70 cause immotility of respiratory cilia and sperm flagella, respectively, as a result of the loss of axonemal outer (ODAs) and inner dynein arms (IDAs), indicating that C11orf70 is involved in cytoplasmic assembly of dynein arms. Expression analyses of C11orf70 showed that C11orf70 is expressed in ciliated respiratory cells and that the expression of C11orf70 is upregulated during ciliogenesis, similar to other previously described cytoplasmic dynein-arm assembly factors. Furthermore, C11orf70 shows an interaction with cytoplasmic ODA/IDA assembly factor DNAAF2, supporting our hypothesis that C11orf70 is a preassembly factor involved in the pathogenesis of PCD. The identification of additional genetic defects that cause PCD and male infertility is of great importance for the clinic as well as for genetic counselling.

Published

2018

26. Mutations in C11ORF70 cause primary ciliary dyskinesia with randomization of left/right body asymmetry due to outer and inner dynein arm defects

Author

Francesca Santamaria, Gerard W. Dougherty, Niki T. Loges, Tabea Menchen, Petra Pennekamp, Miriam Schmidts, Diana Frank, Laura Venditto, Inga M. Höben, Israel Amirav, Kaman Wu, Rim Hjeij, Maria C. Philipsen, Heymut Omran, Julia Wallmeier, Isabella Aprea, Freerk Prenzel, Kim G. Nielsen, Johanna Raidt, Bernd Dworniczak, and Heike Olbrich

Subjects

Genetics, 0303 health sciences, Cilium, Inner dynein arm, Flagellum, Biology, medicine.disease, Sperm, 3. Good health, Male infertility, Cell biology, 03 medical and health sciences, 0302 clinical medicine, Ciliogenesis, medicine, Motile cilium, 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 caused by defects of motile cilia and sperm flagella. We identified loss-of-function mutations in the open reading frame C11ORF70 in PCD individuals from five distinct families. Transmission electron microscopy analyses and high resolution immunofluorescence microscopy demonstrate that loss-of-function mutations in C11ORF70 cause immotility of respiratory cilia and sperm flagella, respectively, due to loss of axonemal outer (ODAs) and inner dynein arms (IDAs), indicating that C11ORF70 is involved in cytoplasmic assembly of dynein arms. Expression analyses of C11ORF70 showed that C11ORF70 is expressed in ciliated respiratory cells and that the expression of C11ORF70 is upregulated during ciliogenesis, similar to other previously described cytoplasmic dynein arm assembly factors. Furthermore, C11ORF70 shows an interaction with cytoplasmic ODA/IDA assembly factor DNAAF2, supporting our hypothesis that C11ORF70 is a novel preassembly factor involved in the pathogenesis of PCD. The identification of a novel genetic defect that causes PCD and male infertility is of great clinical importance as well as for genetic counselling.

Published

2017

27. Abstracts of the 52nd Workshop for Pediatric Research

Author

Rhea van den Bruck, Patrick P. Weil, Thomas Ziegenhals, Philipp Schreiner, Stefan Juranek, Daniel Gödde, Silvia Vogel, Frauke Schuster, Valerie Orth, Johannes Dörner, Daniel Pembaur, Meike Röper, Stefan Störkel, Hubert Zirngibl, Stefan Wirth, Andreas C. W. Jenke, Jan Postberg, Nikolas Boy, Jana Heringer, Gisela Haege, Esther M. Glahn, Georg F. Hoffmann, Sven F. Garbade, Peter Burgard, Stefan Kölker, Cho-Ming Chao, Faady Yahya, Alena Moiseenko, Amit Shrestha, Negah Ahmadvand, Jennifer Quantius, Jochen Wilhelm, Elie El-Agha, Klaus-Peter Zimmer, Saverio Bellusci, Christian Staufner, Holger Prokisch, Stephan Seeliger, Matthias Müller, Andreas Hippe, Henrik Steinkraus, Roland Wauer, Burkhard Lachmann, Sigrun R. Hofmann, Christian M. Hedrich, Jakob Zierk, Farhad Arzideh, Rainer Haeckel, Wolfgang Rascher, Manfred Rauh, Markus Metzler, Sebastian Thieme, Joanna Bandoła, Cornelia Richter, Martin Ryser, Arshad Jamal, Michelle P. Ashton, Malte von Bonin, Matthias Kuhn, Ezio Bonifacio, Reinhard Berner, Sebastian Brenner, Johanna Hammersen, Cristina Has, Nora Naumann-Bartsch, Daniel Stachel, Dimitra Kiritsi, Stephan Söder, Mathilde Tardieu, Leena Bruckner-Tuderman, Holm Schneider, F. Bohne, D. Langer, R. Cencic, T. Eggermann, U. Zechner, J. Pelletier, F. Zepp, T. Enklaar, D. Prawitt, Martin Pech, Markus Weckmann, Femke-Anouska Heinsen, Andre Franke, Christine Happle, Anna-Maria Dittrich, Gesine Hansen, Oliver Fuchs, Erika von Mutius, Brian G. Oliver, Matthias V. Kopp, Claudia Paret, Alexandra Russo, Johanna Theruvath, Bettina Keller, Khalifa El Malki, Nadine Lehmann, Arthur Wingerter, Marie A. Neu, Gerhold-Ay Aslihan, Wolfgang Wagner, Clemens Sommer, Torsten Pietsch, Larissa Seidmann, Jörg Faber, Felix Schreiner, Merle Ackermann, Michael Michalik, Eva Rother, Andras Bilkei-Gorzo, Ildiko Racz, Laura Bindila, Beat Lutz, Jörg Dötsch, Andreas Zimmer, Joachim Woelfle, Hendrik S. Fischer, Tim L. Ullrich, Christoph Bührer, Christoph Czernik, Gerd Schmalisch, Robert Stein, Judith Hagenbuchner, Ursula Kiechl-Kohlendorfer, Petra Obexer, Michael J. Ausserlechner, Niki T. Loges, Adrien Tobias Frommer, Julia Wallmeier, Heymut Omran, Soner Öner-Sieben, Martina Gimpfl, Jan Rozman, Martin Irmler, Johannes Beckers, Martin Hrabe De Angelis, Adelbert Roscher, Eckhard Wolf, Regina Ensenauer, Karolina Nemes, Michael Frühwald, Martin Hasselblatt, Reiner Siebert, Uwe Kordes, Marcel Kool, Haicui Wang, Holly Hardy, Osama Refai, Katy E. S. Barwick, Holly H. Zimmerman, Joachim Weis, Emma L. Baple, Andrew H. Crosby, Sebahattin Cirak, C. Hellmuth, O. Uhl, M. Standl, J. Heinrich, E. Thiering, B. Koletzko, Lena Blümel, Kornelius Kerl, Daniel Picard, Michael C. Frühwald, Max C. Liebau, Guido Reifenberger, Arndt Borkhardt, Marc Remke, D. Tews, M. Wabitsch, P. Fischer-Posovszky, Mike-Andrew Westhoff, Lisa Nonnenmacher, Julia Langhans, Lukas Schneele, Nancy Trenkler, and Klaus-Michael Debatin

Subjects

0303 health sciences, medicine.medical_specialty, business.industry, Pediatric research, MEDLINE, Pharmaceutical Science, medicine.disease, 03 medical and health sciences, 0302 clinical medicine, 030228 respiratory system, Complementary and alternative medicine, Medicine, Pharmacology (medical), business, Intensive care medicine, 030304 developmental biology, Primary ciliary dyskinesia

Published

2017

28. Ciliary beat pattern and frequency in genetic variants of primary ciliary dyskinesia

Author

Heymut Omran, Jörg Große Onnebrink, Gerard W. Dougherty, Karsten Häffner, Julia Wallmeier, Claudius Werner, Rim Hjeij, Niki T. Loges, Heike Olbrich, Petra Pennekamp, and Johanna Raidt

Subjects

Pulmonary and Respiratory Medicine, Genetics, Mutation, Pathology, medicine.medical_specialty, Genetic disorder, Heterozygote advantage, Biology, medicine.disease_cause, medicine.disease, LRRC50, Genetic variation, Genotype, medicine, Allele frequency, Primary ciliary dyskinesia

Abstract

Primary ciliary dyskinesia (PCD) is a rare genetic disorder leading to recurrent respiratory tract infections. High-speed video-microscopy analysis (HVMA) of ciliary beating, currently the first-line diagnostic tool for PCD in most centres, is challenging because recent studies have expanded the spectrum of HVMA findings in PCD from grossly abnormal to very subtle. The objective of this study was to describe the diversity of HVMA findings in genetically confirmed PCD individuals.HVMA was performed as part of the routine work-up of individuals with suspected PCD. Subsequent molecular analysis identified biallelic mutations in the PCD-related genes of 66 individuals. 1072 videos of these subjects were assessed for correlation with the genotype.Biallelic mutations (19 novel) were found in 17 genes: DNAI1, DNAI2, DNAH5, DNAH11, CCDC103, ARMC4, KTU/DNAAF2, LRRC50/DNAAF1, LRRC6, DYX1C1, ZMYND10, CCDC39, CCDC40, CCDC164, HYDIN, RSPH4A and RSPH1. Ciliary beat pattern variations correlated well with the genetic findings, allowing the classification of typical HVMA findings for different genetic groups. In contrast, analysis of ciliary beat frequency did not result in additional diagnostic impact.In conclusion, this study provides detailed knowledge about the diversity of HVMA findings in PCD and may therefore be seen as a guide to the improvement of PCD diagnostics.

Published

2014

29. 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

30. Primary ciliary dyskinesia caused by loss-of-functionGAS8mutations due to defects of the nexin-dynein regulatory complex

Author

Frank Rommelmann, Holger Thiele, Heymut Omran, June K. Marthin, Oliver Schwartz, Maria C. Philipsen, Petra Pennekamp, Claudius Werner, Kim G. Nielsen, Heike Olbrich, Janine Altmüller, Gerard W. Dougherty, Johanna Raidt, Carolin Cremers, Niki T. Loges, Christine Edelbusch, and Julia Wallmeier

Subjects

Sanger sequencing, Pathology, medicine.medical_specialty, Nexin, Genetic heterogeneity, Dynein, Biology, medicine.disease, Genetic analysis, Phenotype, symbols.namesake, Motile cilium, medicine, symbols, biology.protein, Primary ciliary dyskinesia

Abstract

Introduction Primary Ciliary Dyskiensia (PCD) describes a clinically and genetically heterogeneous group of hereditary disorders characterized by chronic mucopurulent infections of the airways caused by dysfunction of multiple motile cilia. Mutations in > 30 genes have been described to cause PCD. We present a new genetic PCD-variant caused by defects of the nexin-dynein regulatory complex (N-DRC). Objectives PCD is widely underdiagnosed because of the great heterogeneity of phenotypes. We wanted to reveal rare PCD-variants with only subtle changes in ciliary beating or ultrastructure by further methods such as immunofluorescence microscopy (IF) and genetic analysis. Methods Patient material was supplied for routine diagnostic work-up including high-speed videomicroscopy (HVMA), transmission electron microscopy (TEM), IF and genetics. Within IF we used an antibody directed against the protein GAS8 (human DRC4). In case of abnormal results we performed whole-exome sequencing and confirmed findings with Sanger sequencing. Results IF showed the absence of GAS8 from the ciliary axoneme in three patients. We excluded mutations in the genes CCDC65 and CCDC164 , which lead to isolated nexin link-defects. Subsequent genetic analysis showed recessive loss-of-function mutations in GAS8 encoding for human protein DRC4 in the three families . HVMA and TEM did not show obvious abnormalities. Conclusions Defects of the N-DRC were difficult to diagnose because routinely performed HVMA and TEM showed almost normal findings. We could show that IF and genetic analysis in those patients can be very useful to detect rare PCD-variants e.g. with defects of the N-DRCs.

Published

2016

31. DYNC2H1 mutation causes Jeune syndrome and recurrent lung infections associated with ciliopathy

Author

Heike Olbrich, Julia Wallmeier, Heymut Omran, Ugur Ozcelik, and Nagehan Emiralioglu

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, Cytoplasmic Dyneins, Male, Pathology, medicine.medical_specialty, Ellis-Van Creveld Syndrome, DNA Mutational Analysis, Video microscopy, Ciliopathies, 03 medical and health sciences, 0302 clinical medicine, Fatal Outcome, Microscopy, Electron, Transmission, Recurrence, medicine, Immunology and Allergy, Humans, Cilia, Respiratory Tract Infections, Genetics (clinical), Ellis–van Creveld syndrome, business.industry, Cilium, Dystrophy, Infant, DNA, medicine.disease, Ciliopathy, 030104 developmental biology, Mutation, Motile cilium, Ciliary Motility Disorders, Radiography, Thoracic, business, Tomography, X-Ray Computed, 030217 neurology & neurosurgery

Abstract

Asphyxiating thoracic dystrophy, also known as Jeune syndrome, is included in a group of syndromic skeletal ciliopathies associated with mutations in genes encoding proteins involved in the formation or function of motile cilia. Herein, we report a 6-mo-old male admitted to hospital with recurrent lung infections, thoracic dystrophy, and respiratory distress that was diagnosed as Jeune syndrome; DYNC2H1 mutation was detected via genetic analysis and ciliary dysfunction was noted via high-speed video microscopy.

Published

2016

32. ENT manifestations in patients with primary ciliary dyskinesia: prevalence and significance of otorhinolaryngologic co-morbidities

Author

Julia Wallmeier, J. Ulrich Sommer, Boris A. Stuck, Heike Olbrich, Heymut Omran, Karl Hörmann, Andreas Blum, and Kerstin Schäfer

Subjects

Adult, Male, medicine.medical_specialty, Pediatrics, Adolescent, Comorbidity, Disease, Young Adult, Germany, Surveys and Questionnaires, Prevalence, medicine, Humans, Medical history, Sinusitis, Child, Rhinitis, Primary ciliary dyskinesia, Kartagener Syndrome, business.industry, General Medicine, medicine.disease, Surgery, Otitis Media, Paranasal sinuses, medicine.anatomical_structure, Otitis, Otorhinolaryngology, Female, medicine.symptom, business

Abstract

Primary ciliary dyskinesia (PCD) is a rare inherited disease with a prevalence of about 1:20,000. The underlying pathogenesis is disrupted ciliary function, which results in delayed mucus transportation leading to chronic inflammation, mainly in the upper and lower respiratory tract. Although the pathogenesis of the disease and its clinical presentation is somewhat understood, data regarding the prevalence of accompanying symptoms is limited, especially in the field of otorhinolaryngology. A total of 44 patients diagnosed with PCD answered a questionnaire regarding the diagnosis and clinical presentation of the disease, their medical history and clinical manifestations, and medical treatment in the field of otorhinolaryngology. The majority of participants (70%) had seen a physician more than 50 times before the diagnosis was made at an average age of 10.9 ± 14.4 years. As much as 59% of all patients had recurring problems at the paranasal sinuses and 69% of these patients needed corresponding surgical intervention. Even more patients (81%) suffered from recurring otitis media and, as a result, 78% of these patients underwent paracentesis with temporary tympanostomy tubes at least once at an average age of 9.5 ± 13.0 years. Otorhinolaryngologic symptoms, especially chronic otitis media and chronic rhinosinusitis, are frequently associated with PCD. Surgical intervention to treat these symptoms is common. The awareness of this disease should be raised, especially among ENT physicians, and surgical intervention should be indicated carefully.

Published

2010

33. Immunofluorescence analysis and diagnosis of primary ciliary dyskinesia with radial spoke defects

Author

Adrien Frommer, Johanna Raidt, Julia Wallmeier, Christine Edelbusch, June Kehelet Marthin, Kim G. Nielsen, Karsten Haeffner, Yasin Memari, Niki T. Loges, Kerem Eitan, Heymut Omran, Mieke Boon, Sandra Cindric, Claudius Werner, Heike Olbrich, Irael Amirav, David Shoseyov, Martine Jaspers, Charlotte Jahnke, Jörg Große Onnebrink, and Rim Hjeij

Subjects

Genetics, Pathology, medicine.medical_specialty, medicine.diagnostic_test, Genetic heterogeneity, Cilium, Radial spoke head, Biology, Immunofluorescence, medicine.disease, Situs inversus, otorhinolaryngologic diseases, medicine, Missense mutation, Gene, Primary ciliary dyskinesia

Abstract

Primary ciliary dyskinesia (PCD) is a genetically heterogeneous recessive disorder caused by several distinct defects in genes responsible for ciliary beating leading to defective mucociliary clearance often associated with randomization of left/right body asymmetry. PCD individuals with defective radial spoke heads are difficult to diagnose due to lack of gross ultrastructural defects and absence of situs inversus . Thus far, most radial spoke mutations identified are loss-of function mutations, and missense variants have been rarely described. Using immunofluorescence analyses (IF), we studied the consequences of different RSPH9 , RSPH4A , and RSPH1 mutations on the assembly of the radial spoke complex to improve diagnostics in PCD. We identified bi-allelic mutations in RSPH9, RSPH4A and RSPH1 including 7 novel mutations comprising missense variants in 21 PCD individuals (16 families). We performed IF using antibodies directed against the radial spoke head components RSPH9, RSPH1 and RSPH4A to analyzed respiratory cilia of these patients. Absence of RSPH4A due to mutations in RSPH4A results in deficient axonemal assembly of the radial spoke head components RSPH1 and RSPH9. RSPH1 mutant cilia, lacking RSPH1 fail to assemble RSPH9, while RSPH9 mutations result in axonemal absence of RSPH9 but do not affect the assembly of the other head proteins RSPH1 and RSPH4A. Interestingly, our results were identical in individuals carrying loss-of-function mutations, missense variants or one amino acid deletion. Thus, we conclude that Immunofluorescence analysis can improve diagnosis of PCD in patients with loss-of-function mutations as well as missense variants.

Published

2015

34. Identification of distinct ciliary beat pattern abnormalities by high-speed video microscopy in primary ciliary dyskinesia

Author

Gerard W. Dougherty, Claudius Werner, Karsten Häffner, Heymut Omran, Rim Hjeij, Heike Olbrich, Petra Pennekamp, Johanna Raidt, Jörg Große Onnebrink, Julia Wallmeier, and Niki T. Loges

Subjects

Pathology, medicine.medical_specialty, Nexin, biology, business.industry, Mucociliary clearance, Cilium, medicine.disease, Genotype, medicine, biology.protein, Abnormal ciliary motility, Respiratory system, Outer dynein arm, business, Primary ciliary dyskinesia

Abstract

Introduction: Primary Ciliary Dyskinesia (PCD) is a rare, genetically heterogenous disorder leading to recurrent respiratory tract infections due to abnormal ciliary motility causing impaired mucociliary clearance. High-speed videomicroscopy analysis (HVMA) of ciliary beat pattern (CBP) and frequency as the current first-line diagnostic tool is an increasing challenge, because current studies widely expended the spectrum of HVMA findings from very subtle to markedly abnormal. Objectives: We assigned typical HVMA findings to genetically confirmed PCD individuals in order to identify typical patterns for various PCD variants. Methods: We assessed 1072 videos from nasal brush biopsies of 66 PCD individuals by HVMA as part of routine diagnostic work-up. HVMA findings were subsequently correlated with the genotype (biallelic mutations in 17 genes). Results: Distinct CBP correlated well with genetic findings, which allows the classification of typical HVMA findings for various genetic groups: Respiratory cilia with outer dynein arm defects (ODA) showed minimal residual movements with a minority of cilia being completely immotile. Cilia with combined inner (IDA) and ODA defects were completely immotile. Defects of the central pair apparatus resulted in a rigid and uncoordinated CBP. Combined IDA and microtubular disorganization defects resulted in a hyperkinetic, very stiff and vibratory CBP. Nexin link defects showed an almost regular CBP with only slightly reduced beating amplitude. Conclusion: This study improves clinical PCD diagnostics by classifying different PCD subtypes using HVMA as the first-line diagnostic tool and facilitates the subsequent diagnostics.

Published

2015

35. Subcellular Analysis of the Motor Protein Apparatus in Ependymal Cilia

Author

Heymut Omran, Petra Pennekamp, N. T. Loges, Gerard W. Dougherty, H. Olbrich, Julia Wallmeier, and Oliver Schwartz

Subjects

Motor protein, business.industry, Cilium, Pediatrics, Perinatology and Child Health, Medicine, Neurology (clinical), General Medicine, business, Cell biology

Published

2015

36. Immunofluorescence Analysis and Diagnosis of Primary Ciliary Dyskinesia with Radial Spoke Defects

Author

Kim G. Nielsen, Adrien Frommer, Julia Wallmeier, Martine Jaspers, David Shoseyov, Karsten Haeffner, June K. Marthin, Claudius Werner, Rim Hjeij, Heike Olbrich, Israel Amirav, Heymut Omran, Richard Durbin, Johanna Raidt, Sandra Cindric, Nael Elias, Sascha Sauer, Yasin Memari, Anja Kolb-Kokocinski, Niki T. Loges, Jörg Große-Onnebrink, Christine Edelbusch, Charlotte Jahnke, Eitan Kerem, and Mieke Boon

Subjects

Pulmonary and Respiratory Medicine, Adult, Male, Adolescent, Clinical Biochemistry, DNA Mutational Analysis, Mutation, Missense, Biology, Immunofluorescence, Young Adult, medicine, otorhinolaryngologic diseases, Missense mutation, Humans, Child, Fluorescent Antibody Technique, Indirect, Molecular Biology, Gene, Primary ciliary dyskinesia, Original Research, Genetics, medicine.diagnostic_test, Genetic heterogeneity, Kartagener Syndrome, Cilium, Proteins, Cell Biology, medicine.disease, DNA-Binding Proteins, Situs inversus, Cytoskeletal Proteins, Child, Preschool, Female, Protein Multimerization

Abstract

Primary ciliary dyskinesia (PCD) is a genetically heterogeneous recessive disorder caused by several distinct defects in genes responsible for ciliary beating, leading to defective mucociliary clearance often associated with randomization of left/right body asymmetry. Individuals with PCD caused by defective radial spoke (RS) heads are difficult to diagnose owing to lack of gross ultrastructural defects and absence of situs inversus. Thus far, most mutations identified in human radial spoke genes (RSPH) are loss-of-function mutations, and missense variants have been rarely described. We studied the consequences of different RSPH9, RSPH4A, and RSPH1 mutations on the assembly of the RS complex to improve diagnostics in PCD. We report 21 individuals with PCD (16 families) with biallelic mutations in RSPH9, RSPH4A, and RSPH1, including seven novel mutations comprising missense variants, and performed high-resolution immunofluorescence analysis of human respiratory cilia. Missense variants are frequent genetic defects in PCD with RS defects. Absence of RSPH4A due to mutations in RSPH4A results in deficient axonemal assembly of the RS head components RSPH1 and RSPH9. RSPH1 mutant cilia, lacking RSPH1, fail to assemble RSPH9, whereas RSPH9 mutations result in axonemal absence of RSPH9, but do not affect the assembly of the other head proteins, RSPH1 and RSPH4A. Interestingly, our results were identical in individuals carrying loss-of-function mutations, missense variants, or one amino acid deletion. Immunofluorescence analysis can improve diagnosis of PCD in patients with loss-of-function mutations as well as missense variants. RSPH4A is the core protein of the RS head.

Published

2015

37. MCIDAS mutations result in a mucociliary clearance disorder with reduced generation of multiple motile cilia

Author

Avraham Avital, Heymut Omran, Chris Kintner, Gerard W. Dougherty, Revital Abitbul, Ruth Soferman, Kris De Boeck, Martine Jaspers, Julia Wallmeier, Heike Olbrich, Marja W. Wessels, Harry Cuppens, Sabine Van daele, Hannah M. Mitchison, Niki T. Loges, Israel Amirav, Eduardo Moya, Claudius Werner, Mieke Boon, Mark Jorissen, Eddie M.K. Chung, Andrew Rutman, Christopher O'Callaghan, Johanna Raidt, Lina Ma, Avigdor Hevroni, and Robert A. Hirst

Subjects

Adult, Male, Cdc20 Proteins, Mucociliary clearance, Cellular differentiation, Cell, General Physics and Astronomy, Physiology, Cell Cycle Proteins, Biology, General Biochemistry, Genetics and Molecular Biology, DNA Glycosylases, Motor protein, Young Adult, Microscopy, Electron, Transmission, medicine, Humans, Cilia, Primary ciliary dyskinesia, Multidisciplinary, Kartagener Syndrome, Cilium, Nuclear Proteins, Cell Differentiation, Forkhead Transcription Factors, General Chemistry, medicine.disease, Pedigree, Cell biology, medicine.anatomical_structure, Gene Expression Regulation, Mucociliary Clearance, Deuterosome, Mutation, Motile cilium, Chromosomes, Human, Pair 5, Female, Ciliary Motility Disorders, Transcription Factors

Abstract

Reduced generation of multiple motile cilia (RGMC) is a rare mucociliary clearance disorder. Affected persons suffer from recurrent infections of upper and lower airways because of highly reduced numbers of multiple motile respiratory cilia. Here we report recessive loss-of-function and missense mutations in MCIDAS-encoding Multicilin, which was shown to promote the early steps of multiciliated cell differentiation in Xenopus. MCIDAS mutant respiratory epithelial cells carry only one or two cilia per cell, which lack ciliary motility-related proteins (DNAH5; CCDC39) as seen in primary ciliary dyskinesia. Consistent with this finding, FOXJ1-regulating axonemal motor protein expression is absent in respiratory cells of MCIDAS mutant individuals. CCNO, when mutated known to cause RGMC, is also absent in MCIDAS mutant respiratory cells, consistent with its downstream activity. Thus, our findings identify Multicilin as a key regulator of CCNO/FOXJ1 for human multiciliated cell differentiation, and highlight the 5q11 region containing CCNO and MCIDAS as a locus underlying RGMC.

Published

2014

38. Mutations in CCDC11, which encodes a coiled-coil containing ciliary protein, causes situs inversus due to dysmotility of monocilia in the left-right organizer

Author

Sudipto Roy, Rim Hjeij, Surin Kumar Thamilselvam, Cordula Koerner-Rettberg, Julia Wallmeier, Heymut Omran, Petra Pennekamp, Niki T. Loges, Semil P. Choksi, Claudius Werner, Adrian Boey, Shubha Vij, and Vijayashankaranarayanan Narasimhan

Subjects

Embryo, Nonmammalian, Motility, Biology, Intraflagellar transport, Genetics, medicine, Basal body, Animals, Humans, Cilia, Zebrafish, Genetics (clinical), Cilium, Embryo, Anatomy, Zebrafish Proteins, medicine.disease, biology.organism_classification, Situs Inversus, Cell biology, Situs inversus, Cytoskeletal Proteins, Disease Models, Animal, Mutation, Motile cilium, Ciliary Motility Disorders

Abstract

In vertebrates, establishment of left-right (LR) asymmetry is dependent on cilia-driven fluid flow within the LR organizer. Mutations in CCDC11 disrupt LR asymmetry in humans, but how the gene functions in LR patterning is presently unknown. We describe a patient with situs inversus totalis carrying homozygous loss-of-function mutations in CCDC11. We show that CCDC11 is an axonemal protein in respiratory cilia, but is largely dispensable for their structure and motility. To investigate the role of CCDC11 in LR development, we studied the zebrafish homolog of the gene. Like in human respiratory cilia, loss of Ccdc11 causes minor defects in the motility of zebrafish kidney cilia, although the protein localizes to their axonemes and base. By contrast, Ccdc11 localizes exclusively to the basal bodies of cilia within Kupffer's vesicle, the organ of laterality of teleost fishes, and within the spinal canal. Moreover, the rotational motion of the cilia in these tissues of ccdc11-deficient embryos was strongly impaired. Our findings demonstrate that CCDC11 has a conserved essential function in cilia of the vertebrate LR organizer. To the best of our knowledge, this is the first ciliary component, which has a differential localization and function in different kinds of motile cilia.

Published

2014

39. Mutations in CCNO result in congenital mucociliary clearance disorder with reduced generation of multiple motile cilia

Author

Gerard W. Dougherty, Lina Ma, Chris Kintner, Gabriele Köhler, Heymut Omran, Cordula Koerner-Rettberg, Petra Pennekamp, Julia Wallmeier, Sabina Schmitt-Grohé, Dalal A. Al-Mutairi, Claudius Werner, Matthias Griese, Tabea Menchen, Mieke Boon, Fowzan S. Alkuraya, Chun-Ting Chen, Martine Jaspers, Elisabeth Horak, Niki T. Loges, Heike Olbrich, Theodor Zimmermann, Basel H Alsabah, and Hanan E. Shamseldin

Subjects

Adult, Male, Cytoplasm, Centriole, Adolescent, Mucociliary clearance, Molecular Sequence Data, Biology, DNA Glycosylases, Motor protein, Mice, Xenopus laevis, Cell Movement, Ciliogenesis, Genetics, Animals, Humans, Amino Acid Sequence, Cilia, Apical cytoplasm, Child, Centrioles, Models, Genetic, Sequence Homology, Amino Acid, Kartagener Syndrome, Cilium, Sequence Analysis, DNA, Cell biology, Pedigree, Deuterosome, Mucociliary Clearance, Child, Preschool, Mutation, Motile cilium, Female

Abstract

Using a whole-exome sequencing strategy, we identified recessive CCNO (encoding cyclin O) mutations in 16 individuals suffering from chronic destructive lung disease due to insufficient airway clearance. Respiratory epithelial cells showed a marked reduction in the number of multiple motile cilia (MMC) covering the cell surface. The few residual cilia that correctly expressed axonemal motor proteins were motile and did not exhibit obvious beating defects. Careful subcellular analyses as well as in vitro ciliogenesis experiments in CCNO-mutant cells showed defective mother centriole generation and placement. Morpholino-based knockdown of the Xenopus ortholog of CCNO also resulted in reduced MMC and centriole numbers in embryonic epidermal cells. CCNO is expressed in the apical cytoplasm of multiciliated cells and acts downstream of multicilin, which governs the generation of multiciliated cells. To our knowledge, CCNO is the first reported gene linking an inherited human disease to reduced MMC generation due to a defect in centriole amplification and migration.

Published

2013