Modelling autosomal dominant optic atrophy associated with OPA1 variants in iPSC-derived retinal ganglion cells

Autosomal dominant optic atrophy (DOA) is the most common inherited optic neuropathy, characterized by the preferential loss of retinal ganglion cells (RGCs), resulting in optic nerve degeneration and progressive bilateral central vision loss. More than 60% of genetically confirmed patients with DOA...

Descripción completa

Detalles Bibliográficos
Autores principales: Sladen, Paul E, Jovanovic, Katarina, Guarascio, Rosellina, Ottaviani, Daniele, Salsbury, Grace, Novoselova, Tatiana, Chapple, J Paul, Yu-Wai-Man, Patrick, Cheetham, Michael E
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2022
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9558835/
https://www.ncbi.nlm.nih.gov/pubmed/35652445
http://dx.doi.org/10.1093/hmg/ddac128
_version_ 1784807531082678272
author Sladen, Paul E
Jovanovic, Katarina
Guarascio, Rosellina
Ottaviani, Daniele
Salsbury, Grace
Novoselova, Tatiana
Chapple, J Paul
Yu-Wai-Man, Patrick
Cheetham, Michael E
author_facet Sladen, Paul E
Jovanovic, Katarina
Guarascio, Rosellina
Ottaviani, Daniele
Salsbury, Grace
Novoselova, Tatiana
Chapple, J Paul
Yu-Wai-Man, Patrick
Cheetham, Michael E
author_sort Sladen, Paul E
collection PubMed
description Autosomal dominant optic atrophy (DOA) is the most common inherited optic neuropathy, characterized by the preferential loss of retinal ganglion cells (RGCs), resulting in optic nerve degeneration and progressive bilateral central vision loss. More than 60% of genetically confirmed patients with DOA carry variants in the nuclear OPA1 gene, which encodes for a ubiquitously expressed, mitochondrial GTPase protein. OPA1 has diverse functions within the mitochondrial network, facilitating inner membrane fusion and cristae modelling, regulating mitochondrial DNA maintenance and coordinating mitochondrial bioenergetics. There are currently no licensed disease-modifying therapies for DOA and the disease mechanisms driving RGC degeneration are poorly understood. Here, we describe the generation of isogenic, heterozygous OPA1 null induced pluripotent stem cell (iPSC) (OPA1+/−) through clustered regularly interspaced short palindromic repeats (CRISPR)/Cas9 gene editing of a control cell line, in conjunction with the generation of DOA patient-derived iPSC carrying OPA1 variants, namely, the c.2708_2711delTTAG variant (DOA iPSC), and previously reported missense variant iPSC line (c.1334G>A, DOA plus [DOA]+ iPSC) and CRISPR/Cas9 corrected controls. A two-dimensional (2D) differentiation protocol was used to study the effect of OPA1 variants on iPSC-RGC differentiation and mitochondrial function. OPA1+/−, DOA and DOA+ iPSC showed no differentiation deficit compared to control iPSC lines, exhibiting comparable expression of all relevant markers at each stage of differentiation. OPA1+/− and OPA1 variant iPSC-RGCs exhibited impaired mitochondrial homeostasis, with reduced bioenergetic output and compromised mitochondrial DNA maintenance. These data highlight mitochondrial deficits associated with OPA1 dysfunction in human iPSC-RGCs, and establish a platform to study disease mechanisms that contribute to RGC loss in DOA, as well as potential therapeutic interventions.
format Online
Article
Text
id pubmed-9558835
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Oxford University Press
record_format MEDLINE/PubMed
spelling pubmed-95588352022-10-18 Modelling autosomal dominant optic atrophy associated with OPA1 variants in iPSC-derived retinal ganglion cells Sladen, Paul E Jovanovic, Katarina Guarascio, Rosellina Ottaviani, Daniele Salsbury, Grace Novoselova, Tatiana Chapple, J Paul Yu-Wai-Man, Patrick Cheetham, Michael E Hum Mol Genet Original Article Autosomal dominant optic atrophy (DOA) is the most common inherited optic neuropathy, characterized by the preferential loss of retinal ganglion cells (RGCs), resulting in optic nerve degeneration and progressive bilateral central vision loss. More than 60% of genetically confirmed patients with DOA carry variants in the nuclear OPA1 gene, which encodes for a ubiquitously expressed, mitochondrial GTPase protein. OPA1 has diverse functions within the mitochondrial network, facilitating inner membrane fusion and cristae modelling, regulating mitochondrial DNA maintenance and coordinating mitochondrial bioenergetics. There are currently no licensed disease-modifying therapies for DOA and the disease mechanisms driving RGC degeneration are poorly understood. Here, we describe the generation of isogenic, heterozygous OPA1 null induced pluripotent stem cell (iPSC) (OPA1+/−) through clustered regularly interspaced short palindromic repeats (CRISPR)/Cas9 gene editing of a control cell line, in conjunction with the generation of DOA patient-derived iPSC carrying OPA1 variants, namely, the c.2708_2711delTTAG variant (DOA iPSC), and previously reported missense variant iPSC line (c.1334G>A, DOA plus [DOA]+ iPSC) and CRISPR/Cas9 corrected controls. A two-dimensional (2D) differentiation protocol was used to study the effect of OPA1 variants on iPSC-RGC differentiation and mitochondrial function. OPA1+/−, DOA and DOA+ iPSC showed no differentiation deficit compared to control iPSC lines, exhibiting comparable expression of all relevant markers at each stage of differentiation. OPA1+/− and OPA1 variant iPSC-RGCs exhibited impaired mitochondrial homeostasis, with reduced bioenergetic output and compromised mitochondrial DNA maintenance. These data highlight mitochondrial deficits associated with OPA1 dysfunction in human iPSC-RGCs, and establish a platform to study disease mechanisms that contribute to RGC loss in DOA, as well as potential therapeutic interventions. Oxford University Press 2022-06-02 /pmc/articles/PMC9558835/ /pubmed/35652445 http://dx.doi.org/10.1093/hmg/ddac128 Text en © The Author(s) 2022. Published by Oxford University Press. https://creativecommons.org/licenses/by/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/), which permits unrestricted reuse, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Article
Sladen, Paul E
Jovanovic, Katarina
Guarascio, Rosellina
Ottaviani, Daniele
Salsbury, Grace
Novoselova, Tatiana
Chapple, J Paul
Yu-Wai-Man, Patrick
Cheetham, Michael E
Modelling autosomal dominant optic atrophy associated with OPA1 variants in iPSC-derived retinal ganglion cells
title Modelling autosomal dominant optic atrophy associated with OPA1 variants in iPSC-derived retinal ganglion cells
title_full Modelling autosomal dominant optic atrophy associated with OPA1 variants in iPSC-derived retinal ganglion cells
title_fullStr Modelling autosomal dominant optic atrophy associated with OPA1 variants in iPSC-derived retinal ganglion cells
title_full_unstemmed Modelling autosomal dominant optic atrophy associated with OPA1 variants in iPSC-derived retinal ganglion cells
title_short Modelling autosomal dominant optic atrophy associated with OPA1 variants in iPSC-derived retinal ganglion cells
title_sort modelling autosomal dominant optic atrophy associated with opa1 variants in ipsc-derived retinal ganglion cells
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9558835/
https://www.ncbi.nlm.nih.gov/pubmed/35652445
http://dx.doi.org/10.1093/hmg/ddac128
work_keys_str_mv AT sladenpaule modellingautosomaldominantopticatrophyassociatedwithopa1variantsinipscderivedretinalganglioncells
AT jovanovickatarina modellingautosomaldominantopticatrophyassociatedwithopa1variantsinipscderivedretinalganglioncells
AT guarasciorosellina modellingautosomaldominantopticatrophyassociatedwithopa1variantsinipscderivedretinalganglioncells
AT ottavianidaniele modellingautosomaldominantopticatrophyassociatedwithopa1variantsinipscderivedretinalganglioncells
AT salsburygrace modellingautosomaldominantopticatrophyassociatedwithopa1variantsinipscderivedretinalganglioncells
AT novoselovatatiana modellingautosomaldominantopticatrophyassociatedwithopa1variantsinipscderivedretinalganglioncells
AT chapplejpaul modellingautosomaldominantopticatrophyassociatedwithopa1variantsinipscderivedretinalganglioncells
AT yuwaimanpatrick modellingautosomaldominantopticatrophyassociatedwithopa1variantsinipscderivedretinalganglioncells
AT cheethammichaele modellingautosomaldominantopticatrophyassociatedwithopa1variantsinipscderivedretinalganglioncells

Ejemplares similares