PRUNE1 Deficiency: Expanding the Clinical and Genetic Spectrum-Reference-Cited by-同舟云学术

PRUNE1 Deficiency: Expanding the Clinical and Genetic Spectrum

Published:2018-06-25 Issue:05 Volume:49 Page:330-338
ISSN:0174-304X
Container-title:Neuropediatrics
language:en
Short-container-title:Neuropediatrics

Author:

Schossig Anna¹,Haack Tobias²³⁴,Kovács-Nagy Reka²,Braunisch Matthias²⁵,Makowski Christine⁶,Senderek Jan⁷,Vill Katharina⁸,Müller-Felber Wolfgang⁸,Strom Tim²³,Krabichler Birgit¹,Freisinger Peter⁹,Deshpande Charu¹⁰,Polster Tilman¹¹,Wolf Nicole¹²,Desguerre Isabelle¹³,Wörmann Friedrich¹¹,Rötig Agnès¹⁴,Ahting Uwe²,Kopajtich Robert²³,Prokisch Holger²³,Meitinger Thomas²³,Feichtinger René¹⁵,Mayr Johannes¹⁵,Jungbluth Heinz¹⁶¹⁷¹⁸,Hubmann Michael¹⁹,Zschocke Johannes¹,Distelmaier Felix²⁰,Koch Johannes¹⁵,Alhaddad Bader²

Affiliation:

1. Division of Human Genetics, Medical University Innsbruck, Innsbruck, Austria

2. Institute of Human Genetics, Klinikum rechts der Isar, Technische Universität München, Munich, Germany

3. Institute of Human Genetics, Helmholtz Zentrum München, Neuherberg, Germany

4. Institute of Medical Genetics and Applied Genomics, University of Tübingen, Germany

5. Department of Nephrology, Klinikum rechts der Isar, Technische Universität München, Munich, Germany

6. Department of Pediatrics, Technische Universität München (TUM), Munich, Germany

7. Department of Neurology, Friedrich Baur Institute, Ludwig Maximilians University Munich, Munich, Germany

8. Department of Pediatric Neurology and Developmental Medicine, Dr. v. Hauner Children's Hospital, Ludwig-Maximilians-Universität München, Munich, Germany

9. Department of Pediatrics, Kreisklinken Reutlingen, Reutlingen, Germany

10. Department of Clinical Genetics, Guy's Hospital, London, United Kingdom

11. Department of Pediatric Epileptology, Bethel Epilepsy Centre, Bielefeld, Germany

12. Department of Child Neurology and Amsterdam Neuroscience, VU University Medical Centre, Amsterdam, The Netherlands

13. Department of Pediatric Neurology, Necker Enfants Malades Hospital, Paris, France

14. INSERM U1163, Institut Imagine, Université Paris Descartes, Paris, France

15. Department of Pediatrics, Salzburger Landeskliniken (SALK) and Paracelsus Medical University (PMU), Salzburg, Austria

16. Department of Paediatric Neurology, Neuromuscular Service, Evelina's Children Hospital, Guy's & St. Thomas' Hospital NHS Foundation Trust, London, United Kingdom

17. Randall Division of Cell and Molecular Biophysics, Muscle Signalling Section, King's College, London, United Kingdom

18. Department of Basic and Clinical Neuroscience, IoPPN, King's College London, London, United Kingdom

19. Department of Neuropediatrics, Kinderärzte Zirndorf, Zirndorf, Germany

20. Department of General Pediatrics, Neonatology and Pediatric Cardiology, University Children's Hospital, Medical Faculty, Heinrich Heine University, Düsseldorf, Germany

Abstract

Background Primary microcephaly and profound global developmental delay have been considered the core clinical phenotype in patients with bi-allelic PRUNE1 mutations. Methods Linkage analysis and whole-exome sequencing (WES) in a multiplex family and extraction of further cases from a WES repository containing 571 children with severe developmental disabilities and neurologic symptoms. Results We identified bi-allelic PRUNE1 mutations in twelve children from six unrelated families. All patients who survived beyond the first 6 months of life had early-onset global developmental delay, bilateral spastic paresis, dysphagia and difficult-to-treat seizures, while congenital or later-evolving microcephaly was not a consistent finding. Brain MRI showed variable anomalies with progressive cerebral and cerebellar atrophies and T2-hyperintense brain stem lesions. Peripheral neuropathy was documented in five cases. Disease course was progressive in all patients and eight children died in the first or early second decade of life. In addition to the previously reported missense mutation p.(Asp106Asn), we observed a novel homozygous missense variant p.(Leu172Pro) and a homozygous contiguous gene deletion encompassing most of the PRUNE1 gene and part of the neighboring BNIPL gene. Conclusions PRUNE1 deficiency causes severe early-onset disease affecting the central and peripheral nervous systems. Microcephaly is probably not a universal feature.

Publisher

Georg Thieme Verlag KG

Subject

Clinical Neurology,General Medicine,Pediatrics, Perinatology, and Child Health

Link

http://www.thieme-connect.de/products/ejournals/pdf/10.1055/s-0038-1661396.pdf

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2. Newborn Screening for SMA – Can a Wait-and-See Strategy be Responsibly Justified in Patients With Four SMN2 Copies?;Journal of Neuromuscular Diseases;2022-09-09

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