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GPATCH11 variants cause mis-splicing and early-onset retinal dystrophy with neurological impairment

Author

Listed:
  • Andrea Zanetti

    (Imagine and Paris Cité University)

  • Gwendal Dujardin

    (EFS)

  • Lucas Fares-Taie

    (Imagine and Paris Cité University)

  • Jeanne Amiel

    (Imagine and Paris Cité University)

  • Jérôme E. Roger

    (Paris-Saclay University)

  • Isabelle Audo

    (National Rare Disease Center REFERET F-)

  • Matthieu P. Robert

    (APHP)

  • Pierre David

    (Imagine)

  • Vincent Jung

    (INSERM US24/CNRS UAR 3633)

  • Nicolas Goudin

    (INSERM US24/CNRS UAR 3633)

  • Ida Chiara Guerrera

    (INSERM US24/CNRS UAR 3633)

  • Stéphanie Moriceau

    (INSERM US24/CNRS UAR 3633, Institute of Genetic Diseases, Imagine)

  • Danielle Amana

    (Hospital Center of Orleans)

  • Nurit Assia Batzir

    (Schneider Children’s Medical Center of Israel)

  • Anat Bachar-Zipori

    (Tel Aviv University)

  • Lina Basel Salmon

    (Tel Aviv University
    Rabin Medical Center
    Felsenstein Medical Research Center)

  • Nathalie Boddaert

    (INSERM UMR1163)

  • Sylvain Briault

    (Regional Hospital of Orleans (CHRO))

  • Ange-Line Bruel

    (CHU Dijon)

  • Christine Costet-Fighiera

    (Centre d’Ophtalmologie M’Eye Clinic
    Clinique St George)

  • Luisa Coutinho Santos

    (Instituto de Oftalmologia Dr. Gama Pinto (IOGP))

  • Cyril Gitiaux

    (Paris Cité University)

  • Karolina Kaminska

    (Institute of Molecular and Clinical Ophthalmology Basel (IOB)
    University of Basel)

  • Paul Kuentz

    (CHU Dijon)

  • Naama Orenstein

    (Schneider Children’s Medical Center of Israel
    Tel Aviv University)

  • Nicole Philip-Sarles

    (Hospital Timone Enfant)

  • Morgane Plutino

    (CHU de Nice)

  • Mathieu Quinodoz

    (Institute of Molecular and Clinical Ophthalmology Basel (IOB)
    University of Basel
    University of Leicester)

  • Cristina Santos

    (Instituto de Oftalmologia Dr. Gama Pinto (IOGP)
    Universidade NOVA de Lisboa)

  • Sabine Sigaudy

    (Hospital Timone Enfant)

  • Mariana Soeiro e Sá

    (Centro Hospitalar Universitário Lisboa Norte)

  • Efrat Sofrin

    (Schneider Children’s Medical Center of Israel)

  • Ana Berta Sousa

    (Centro Hospitalar Universitário Lisboa Norte
    University of Lisbon)

  • Rui Sousa-Luis

    (University of Oxford)

  • Christel Thauvin-Robinet

    (CHU Dijon
    CHU Dijon)

  • Erwin L. van Dijk

    (Institute for Integrative Biology of the Cell (I2BC))

  • Khaoula Zaafrane-Khachnaoui

    (CHU de Nice)

  • Dinah Zur

    (Tel Aviv University)

  • Josseline Kaplan

    (Imagine and Paris Cité University)

  • Carlo Rivolta

    (Institute of Molecular and Clinical Ophthalmology Basel (IOB)
    University of Basel
    University of Leicester)

  • Jean-Michel Rozet

    (Imagine and Paris Cité University)

  • Isabelle Perrault

    (Imagine and Paris Cité University)

Abstract

Here we conduct a study involving 12 individuals with retinal dystrophy, neurological impairment, and skeletal abnormalities, with special focus on GPATCH11, a lesser-known G-patch domain-containing protein, regulator of RNA metabolism. To elucidate its role, we study fibroblasts from unaffected individuals and patients carrying the recurring c.328+1 G > T mutation, which specifically removes the main part of the G-patch domain while preserving the other domains. Additionally, we generate a mouse model replicating the patients’ phenotypic defects, including retinal dystrophy and behavioral abnormalities. Our results reveal a subcellular localization of GPATCH11 characterized by a diffuse presence in the nucleoplasm, as well as centrosomal localization, suggesting potential functions in RNA and cilia metabolism. Transcriptomic analysis performed on mouse retina detect dysregulation in both gene expression and splicing activity, impacting key processes such as photoreceptor light responses, RNA regulation, and primary cilia-associated metabolism. Proteomic analysis of mouse retina confirms the roles GPATCH11 plays in RNA processing, splicing, and transcription regulation, while also suggesting additional functions in synaptic plasticity and nuclear stress response. Our research provides insights into the diverse roles of GPATCH11 and identifies that the mutations affecting this protein are responsible for a recently characterized described syndrome.

Suggested Citation

  • Andrea Zanetti & Gwendal Dujardin & Lucas Fares-Taie & Jeanne Amiel & Jérôme E. Roger & Isabelle Audo & Matthieu P. Robert & Pierre David & Vincent Jung & Nicolas Goudin & Ida Chiara Guerrera & Stépha, 2024. "GPATCH11 variants cause mis-splicing and early-onset retinal dystrophy with neurological impairment," Nature Communications, Nature, vol. 15(1), pages 1-20, December.
  • Handle: RePEc:nat:natcom:v:15:y:2024:i:1:d:10.1038_s41467-024-54549-8
    DOI: 10.1038/s41467-024-54549-8
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    References listed on IDEAS

    as
    1. Yingyao Zhou & Bin Zhou & Lars Pache & Max Chang & Alireza Hadj Khodabakhshi & Olga Tanaseichuk & Christopher Benner & Sumit K. Chanda, 2019. "Metascape provides a biologist-oriented resource for the analysis of systems-level datasets," Nature Communications, Nature, vol. 10(1), pages 1-10, December.
    2. Martina Riva & Stéphanie Moriceau & Annunziato Morabito & Elena Dossi & Candela Sanchez-Bellot & Patrick Azzam & Andrea Navas-Olive & Beatriz Gal & Francesco Dori & Elena Cid & Fanny Ledonne & Sabrina, 2023. "Aberrant survival of hippocampal Cajal-Retzius cells leads to memory deficits, gamma rhythmopathies and susceptibility to seizures in adult mice," Nature Communications, Nature, vol. 14(1), pages 1-21, December.
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