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IFT81, encoding an IFT-B core protein, as a very rare cause of a ciliopathy phenotype
  1. Isabelle Perrault1,2,
  2. Jan Halbritter3,4,
  3. Jonathan D Porath4,
  4. Xavier Gérard1,2,
  5. Daniela A Braun4,
  6. Heon Yung Gee4,
  7. Hanan M Fathy5,
  8. Sophie Saunier2,6,
  9. Valérie Cormier-Daire2,7,
  10. Sophie Thomas2,8,
  11. Tania Attié-Bitach2,8,
  12. Nathalie Boddaert9,
  13. Michael Taschner10,
  14. Markus Schueler4,
  15. Esben Lorentzen10,
  16. Richard P Lifton11,
  17. Jennifer A Lawson4,
  18. Meriem Garfa-Traore2,12,
  19. Edgar A Otto13,
  20. Philippe Bastin14,
  21. Catherine Caillaud15,
  22. Josseline Kaplan1,2,
  23. Jean-Michel Rozet1,2,
  24. Friedhelm Hildebrandt4,16
  1. 1Laboratory of Genetics in Ophthalmology, INSERM UMR 1163, Paris, France
  2. 2Paris Descartes—Sorbonne Paris Cité University, Imagine Institute, Paris, France
  3. 3Division of Endocrinology and Nephrology, Department of Internal Medicine, University Clinic Leipzig, Leipzig, Germany
  4. 4Division of Nephrology, Department of Medicine, Boston Children's Hospital, Harvard Medical School, Boston, Massachusetts, USA
  5. 5Pediatric Nephrology Unit, University of Alexandria, Alexandria, Egypt
  6. 6INSERM UMR 1163, Molecular bases of hereditary kidney diseases, Nephronophthisis and Hypodysplasia, Paris, France
  7. 7INSERM UMR 1163, Molecular and Physiopathological bases of osteochondrodysplasia, Paris, France
  8. 8INSERM UMR 1163, Embryology and genetics of human malformation, Paris, France
  9. 9Department of Pediatric Radiology, Hôpital Necker-Enfants Malades, APHP, Descartes University, Paris, France
  10. 10Department of Structural Cell Biology, Max Planck Institute of Biochemistry, Martinsried, Germany
  11. 11Department of Genetics, Howard Hughes Medical Institute, Yale University School of Medicine, New Haven, USA
  12. 12INSERM UMR 1163, Cell imaging platform, Paris, France
  13. 13Departments of Pediatrics, University of Michigan, Ann Arbor, USA
  14. 14Trypanosome Cell Biology Unit, Institut Pasteur and CNRS, URA 2581, Paris, France
  15. 15Biochemistry Department, Necker Hospital, Paris, France
  16. 16Howard Hughes Medical Institute, Chevy Chase, Maryland, USA
  1. Correspondence to Professor Friedhelm Hildebrandt, Professor of Pediatrics, Harvard Medical School, Director, Division of Nephrology, Investigator, Howard Hughes Medical Institute, Boston Children's Hospital, 300 Longwood Avenue, Boston, MA 02115, USA; friedhelm.hildebrandt{at}childrens.harvard.edu or Dr Jean-Michel Rozet, Director of Research, Head, Laboratory of Genetics in Ophthalmology, INSERM UMR1163, Imagine Institute of Genetic Diseases, 24 boulevard du Montparnasse, 75015 Paris, France; Jean-michel.rozet{at}inserm.fr

Abstract

Background Bidirectional intraflagellar transport (IFT) consists of two major protein complexes, IFT-A and IFT-B. In contrast to the IFT-B complex, all components of IFT-A have recently been linked to human ciliopathies when defective. We therefore hypothesised that mutations in additional IFT-B encoding genes can be found in patients with multisystemic ciliopathies.

Methods We screened 1628 individuals with reno-ocular ciliopathies by targeted next-generation sequencing of ciliary candidate genes, including all IFT-B encoding genes.

Results Consequently, we identified a homozygous mutation in IFT81 affecting an obligatory donor splice site in an individual with nephronophthisis and polydactyly. Further, we detected a loss-of-stop mutation with extension of the deduced protein by 10 amino acids in an individual with neuronal ceroid lipofuscinosis-1. This proband presented with retinal dystrophy and brain lesions including cerebellar atrophy, a phenotype to which the IFT81 variant might contribute. Cultured fibroblasts of this latter affected individual showed a significant decrease in ciliated cell abundance compared with controls and increased expression of the transcription factor GLI2 suggesting deranged sonic hedgehog signalling.

Conclusions This work describes identification of mutations of IFT81 in individuals with symptoms consistent with the clinical spectrum of ciliopathies. It might represent the rare case of a core IFT-B complex protein found associated with human disease. Our data further suggest that defects in the IFT-B core are an exceedingly rare finding, probably due to its indispensable role for ciliary assembly in development.

  • Genetics
  • Molecular genetics
  • Ophthalmology
  • Renal Medicine

This is an Open Access article distributed in accordance with the terms of the Creative Commons Attribution (CC BY 4.0) license, which permits others to distribute, remix, adapt and build upon this work, for commercial use, provided the original work is properly cited. See: http://creativecommons.org/licenses/by/4.0/

https://doi.org/10.1136/jmedgenet-2014-102838

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