Genetic therapy in a mitochondrial disease model suggests a critical role for liver dysfunction in mortality

The clinical and largely unpredictable heterogeneity of phenotypes in patients with mitochondrial disorders demonstrates the ongoing challenges in the understanding of this semi-autonomous organelle in biology and disease. Previously, we used the gene-breaking transposon to create 1200 transgenic ze...

Descripción completa

Detalles Bibliográficos
Autores principales: Sabharwal, Ankit, Wishman, Mark D, Cervera, Roberto Lopez, Serres, MaKayla R, Anderson, Jennifer L, Holmberg, Shannon R, Kar, Bibekananda, Treichel, Anthony J, Ichino, Noriko, Liu, Weibin, Yang, Jingchun, Ding, Yonghe, Deng, Yun, Lacey, Jean M, Laxen, William J, Loken, Perry R, Oglesbee, Devin, Farber, Steven A, Clark, Karl J, Xu, Xiaolei, Ekker, Stephen C
Formato: Online Artículo Texto
Lenguaje:English
Publicado: eLife Sciences Publications, Ltd 2022
Materias:
Developmental Biology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9859037/
https://www.ncbi.nlm.nih.gov/pubmed/36408801
http://dx.doi.org/10.7554/eLife.65488
_version_ 1784874255653011456
author Sabharwal, Ankit
Wishman, Mark D
Cervera, Roberto Lopez
Serres, MaKayla R
Anderson, Jennifer L
Holmberg, Shannon R
Kar, Bibekananda
Treichel, Anthony J
Ichino, Noriko
Liu, Weibin
Yang, Jingchun
Ding, Yonghe
Deng, Yun
Lacey, Jean M
Laxen, William J
Loken, Perry R
Oglesbee, Devin
Farber, Steven A
Clark, Karl J
Xu, Xiaolei
Ekker, Stephen C
author_facet Sabharwal, Ankit
Wishman, Mark D
Cervera, Roberto Lopez
Serres, MaKayla R
Anderson, Jennifer L
Holmberg, Shannon R
Kar, Bibekananda
Treichel, Anthony J
Ichino, Noriko
Liu, Weibin
Yang, Jingchun
Ding, Yonghe
Deng, Yun
Lacey, Jean M
Laxen, William J
Loken, Perry R
Oglesbee, Devin
Farber, Steven A
Clark, Karl J
Xu, Xiaolei
Ekker, Stephen C
author_sort Sabharwal, Ankit
collection PubMed
description The clinical and largely unpredictable heterogeneity of phenotypes in patients with mitochondrial disorders demonstrates the ongoing challenges in the understanding of this semi-autonomous organelle in biology and disease. Previously, we used the gene-breaking transposon to create 1200 transgenic zebrafish strains tagging protein-coding genes (Ichino et al., 2020), including the lrpprc locus. Here, we present and characterize a new genetic revertible animal model that recapitulates components of Leigh Syndrome French Canadian Type (LSFC), a mitochondrial disorder that includes diagnostic liver dysfunction. LSFC is caused by allelic variations in the LRPPRC gene, involved in mitochondrial mRNA polyadenylation and translation. lrpprc zebrafish homozygous mutants displayed biochemical and mitochondrial phenotypes similar to clinical manifestations observed in patients, including dysfunction in lipid homeostasis. We were able to rescue these phenotypes in the disease model using a liver-specific genetic model therapy, functionally demonstrating a previously under-recognized critical role for the liver in the pathophysiology of this disease.
format Online
Article
Text
id pubmed-9859037
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher eLife Sciences Publications, Ltd
record_format MEDLINE/PubMed
spelling pubmed-98590372023-01-21 Genetic therapy in a mitochondrial disease model suggests a critical role for liver dysfunction in mortality Sabharwal, Ankit Wishman, Mark D Cervera, Roberto Lopez Serres, MaKayla R Anderson, Jennifer L Holmberg, Shannon R Kar, Bibekananda Treichel, Anthony J Ichino, Noriko Liu, Weibin Yang, Jingchun Ding, Yonghe Deng, Yun Lacey, Jean M Laxen, William J Loken, Perry R Oglesbee, Devin Farber, Steven A Clark, Karl J Xu, Xiaolei Ekker, Stephen C eLife Developmental Biology The clinical and largely unpredictable heterogeneity of phenotypes in patients with mitochondrial disorders demonstrates the ongoing challenges in the understanding of this semi-autonomous organelle in biology and disease. Previously, we used the gene-breaking transposon to create 1200 transgenic zebrafish strains tagging protein-coding genes (Ichino et al., 2020), including the lrpprc locus. Here, we present and characterize a new genetic revertible animal model that recapitulates components of Leigh Syndrome French Canadian Type (LSFC), a mitochondrial disorder that includes diagnostic liver dysfunction. LSFC is caused by allelic variations in the LRPPRC gene, involved in mitochondrial mRNA polyadenylation and translation. lrpprc zebrafish homozygous mutants displayed biochemical and mitochondrial phenotypes similar to clinical manifestations observed in patients, including dysfunction in lipid homeostasis. We were able to rescue these phenotypes in the disease model using a liver-specific genetic model therapy, functionally demonstrating a previously under-recognized critical role for the liver in the pathophysiology of this disease. eLife Sciences Publications, Ltd 2022-11-21 /pmc/articles/PMC9859037/ /pubmed/36408801 http://dx.doi.org/10.7554/eLife.65488 Text en © 2022, Sabharwal, Wishman, Cervera et al https://creativecommons.org/licenses/by/4.0/This article is distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use and redistribution provided that the original author and source are credited.
spellingShingle Developmental Biology
Sabharwal, Ankit
Wishman, Mark D
Cervera, Roberto Lopez
Serres, MaKayla R
Anderson, Jennifer L
Holmberg, Shannon R
Kar, Bibekananda
Treichel, Anthony J
Ichino, Noriko
Liu, Weibin
Yang, Jingchun
Ding, Yonghe
Deng, Yun
Lacey, Jean M
Laxen, William J
Loken, Perry R
Oglesbee, Devin
Farber, Steven A
Clark, Karl J
Xu, Xiaolei
Ekker, Stephen C
Genetic therapy in a mitochondrial disease model suggests a critical role for liver dysfunction in mortality
title Genetic therapy in a mitochondrial disease model suggests a critical role for liver dysfunction in mortality
title_full Genetic therapy in a mitochondrial disease model suggests a critical role for liver dysfunction in mortality
title_fullStr Genetic therapy in a mitochondrial disease model suggests a critical role for liver dysfunction in mortality
title_full_unstemmed Genetic therapy in a mitochondrial disease model suggests a critical role for liver dysfunction in mortality
title_short Genetic therapy in a mitochondrial disease model suggests a critical role for liver dysfunction in mortality
title_sort genetic therapy in a mitochondrial disease model suggests a critical role for liver dysfunction in mortality
topic Developmental Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9859037/
https://www.ncbi.nlm.nih.gov/pubmed/36408801
http://dx.doi.org/10.7554/eLife.65488
work_keys_str_mv AT sabharwalankit genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT wishmanmarkd genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT cerverarobertolopez genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT serresmakaylar genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT andersonjenniferl genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT holmbergshannonr genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT karbibekananda genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT treichelanthonyj genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT ichinonoriko genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT liuweibin genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT yangjingchun genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT dingyonghe genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT dengyun genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT laceyjeanm genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT laxenwilliamj genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT lokenperryr genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT oglesbeedevin genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT farberstevena genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT clarkkarlj genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT xuxiaolei genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality
AT ekkerstephenc genetictherapyinamitochondrialdiseasemodelsuggestsacriticalroleforliverdysfunctioninmortality

Ejemplares similares