Genetic Background Effects on Disease Onset and Lifespan of the Mutant Dynactin p150(Glued) Mouse Model of Motor Neuron Disease

Amyotrophic lateral sclerosis (ALS) is a neurodegenerative disease primarily affecting motor neurons in the central nervous system. Although most cases of ALS are sporadic, about 5–10% of cases are familial (FALS) with approximately 20% of FALS caused by mutations in the Cu/Zn superoxide dismutase (...

Descripción completa

Detalles Bibliográficos
Autores principales: Heiman-Patterson, Terry D., Blankenhorn, Elizabeth P., Sher, Roger B., Jiang, Juliann, Welsh, Priscilla, Dixon, Meredith C., Jeffrey, Jeremy I., Wong, Philip, Cox, Gregory A., Alexander, Guillermo M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4357475/
https://www.ncbi.nlm.nih.gov/pubmed/25763819
http://dx.doi.org/10.1371/journal.pone.0117848
_version_ 1782361155802497024
author Heiman-Patterson, Terry D.
Blankenhorn, Elizabeth P.
Sher, Roger B.
Jiang, Juliann
Welsh, Priscilla
Dixon, Meredith C.
Jeffrey, Jeremy I.
Wong, Philip
Cox, Gregory A.
Alexander, Guillermo M.
author_facet Heiman-Patterson, Terry D.
Blankenhorn, Elizabeth P.
Sher, Roger B.
Jiang, Juliann
Welsh, Priscilla
Dixon, Meredith C.
Jeffrey, Jeremy I.
Wong, Philip
Cox, Gregory A.
Alexander, Guillermo M.
author_sort Heiman-Patterson, Terry D.
collection PubMed
description Amyotrophic lateral sclerosis (ALS) is a neurodegenerative disease primarily affecting motor neurons in the central nervous system. Although most cases of ALS are sporadic, about 5–10% of cases are familial (FALS) with approximately 20% of FALS caused by mutations in the Cu/Zn superoxide dismutase (SOD1) gene. We have reported that hSOD1-G93A transgenic mice modeling this disease show a more severe phenotype when the transgene is bred on a pure SJL background and a milder phenotype when bred on a pure B6 background and that these phenotype differences link to a region on mouse Chromosome 17.To examine whether other models of motor neuron degeneration are affected by genetic background, we bred the mutant human dynactin p150(Glued) (G59S-hDCTN1) transgene onto inbred SJL and B6 congenic lines. This model is based on an autosomal dominant lower motor neuron disease in humans linked to a mutation in the p150(Glued) subunit of the dynactin complex. As seen in hSOD1-G93A mice, we observed a more severe phenotype with earlier disease onset (p<0.001) and decreased survival (p<0.00001) when the G59S-hDCTN1 transgene was bred onto the SJL background and delayed onset (p<0.0001) with increased survival (p<0.00001) when bred onto the B6 background. Furthermore, B6 mice with an SJL derived chromosome 17 interval previously shown to delay disease onset in hSOD1-G93A mice also showed delays onset in G59S-hDCTN1 mice suggesting that at least some genetic modifiers are shared. We have shown that genetic background influences phenotype in G59S-hDCTN1 mice, in part through a region of chromosome 17 similar to the G93-hSOD1 ALS mouse model. These results support the presence of genetic modifiers in both these models some of which may be shared. Identification of these modifiers will highlight intracellular pathways involved in motor neuron disease and provide new therapeutic targets that may be applicable to motor neuron degeneration.
format Online
Article
Text
id pubmed-4357475
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-43574752015-03-23 Genetic Background Effects on Disease Onset and Lifespan of the Mutant Dynactin p150(Glued) Mouse Model of Motor Neuron Disease Heiman-Patterson, Terry D. Blankenhorn, Elizabeth P. Sher, Roger B. Jiang, Juliann Welsh, Priscilla Dixon, Meredith C. Jeffrey, Jeremy I. Wong, Philip Cox, Gregory A. Alexander, Guillermo M. PLoS One Research Article Amyotrophic lateral sclerosis (ALS) is a neurodegenerative disease primarily affecting motor neurons in the central nervous system. Although most cases of ALS are sporadic, about 5–10% of cases are familial (FALS) with approximately 20% of FALS caused by mutations in the Cu/Zn superoxide dismutase (SOD1) gene. We have reported that hSOD1-G93A transgenic mice modeling this disease show a more severe phenotype when the transgene is bred on a pure SJL background and a milder phenotype when bred on a pure B6 background and that these phenotype differences link to a region on mouse Chromosome 17.To examine whether other models of motor neuron degeneration are affected by genetic background, we bred the mutant human dynactin p150(Glued) (G59S-hDCTN1) transgene onto inbred SJL and B6 congenic lines. This model is based on an autosomal dominant lower motor neuron disease in humans linked to a mutation in the p150(Glued) subunit of the dynactin complex. As seen in hSOD1-G93A mice, we observed a more severe phenotype with earlier disease onset (p<0.001) and decreased survival (p<0.00001) when the G59S-hDCTN1 transgene was bred onto the SJL background and delayed onset (p<0.0001) with increased survival (p<0.00001) when bred onto the B6 background. Furthermore, B6 mice with an SJL derived chromosome 17 interval previously shown to delay disease onset in hSOD1-G93A mice also showed delays onset in G59S-hDCTN1 mice suggesting that at least some genetic modifiers are shared. We have shown that genetic background influences phenotype in G59S-hDCTN1 mice, in part through a region of chromosome 17 similar to the G93-hSOD1 ALS mouse model. These results support the presence of genetic modifiers in both these models some of which may be shared. Identification of these modifiers will highlight intracellular pathways involved in motor neuron disease and provide new therapeutic targets that may be applicable to motor neuron degeneration. Public Library of Science 2015-03-12 /pmc/articles/PMC4357475/ /pubmed/25763819 http://dx.doi.org/10.1371/journal.pone.0117848 Text en © 2015 Heiman-Patterson et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Heiman-Patterson, Terry D.
Blankenhorn, Elizabeth P.
Sher, Roger B.
Jiang, Juliann
Welsh, Priscilla
Dixon, Meredith C.
Jeffrey, Jeremy I.
Wong, Philip
Cox, Gregory A.
Alexander, Guillermo M.
Genetic Background Effects on Disease Onset and Lifespan of the Mutant Dynactin p150(Glued) Mouse Model of Motor Neuron Disease
title Genetic Background Effects on Disease Onset and Lifespan of the Mutant Dynactin p150(Glued) Mouse Model of Motor Neuron Disease
title_full Genetic Background Effects on Disease Onset and Lifespan of the Mutant Dynactin p150(Glued) Mouse Model of Motor Neuron Disease
title_fullStr Genetic Background Effects on Disease Onset and Lifespan of the Mutant Dynactin p150(Glued) Mouse Model of Motor Neuron Disease
title_full_unstemmed Genetic Background Effects on Disease Onset and Lifespan of the Mutant Dynactin p150(Glued) Mouse Model of Motor Neuron Disease
title_short Genetic Background Effects on Disease Onset and Lifespan of the Mutant Dynactin p150(Glued) Mouse Model of Motor Neuron Disease
title_sort genetic background effects on disease onset and lifespan of the mutant dynactin p150(glued) mouse model of motor neuron disease
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4357475/
https://www.ncbi.nlm.nih.gov/pubmed/25763819
http://dx.doi.org/10.1371/journal.pone.0117848
work_keys_str_mv AT heimanpattersonterryd geneticbackgroundeffectsondiseaseonsetandlifespanofthemutantdynactinp150gluedmousemodelofmotorneurondisease
AT blankenhornelizabethp geneticbackgroundeffectsondiseaseonsetandlifespanofthemutantdynactinp150gluedmousemodelofmotorneurondisease
AT sherrogerb geneticbackgroundeffectsondiseaseonsetandlifespanofthemutantdynactinp150gluedmousemodelofmotorneurondisease
AT jiangjuliann geneticbackgroundeffectsondiseaseonsetandlifespanofthemutantdynactinp150gluedmousemodelofmotorneurondisease
AT welshpriscilla geneticbackgroundeffectsondiseaseonsetandlifespanofthemutantdynactinp150gluedmousemodelofmotorneurondisease
AT dixonmeredithc geneticbackgroundeffectsondiseaseonsetandlifespanofthemutantdynactinp150gluedmousemodelofmotorneurondisease
AT jeffreyjeremyi geneticbackgroundeffectsondiseaseonsetandlifespanofthemutantdynactinp150gluedmousemodelofmotorneurondisease
AT wongphilip geneticbackgroundeffectsondiseaseonsetandlifespanofthemutantdynactinp150gluedmousemodelofmotorneurondisease
AT coxgregorya geneticbackgroundeffectsondiseaseonsetandlifespanofthemutantdynactinp150gluedmousemodelofmotorneurondisease
AT alexanderguillermom geneticbackgroundeffectsondiseaseonsetandlifespanofthemutantdynactinp150gluedmousemodelofmotorneurondisease

Ejemplares similares