A Hypomorphic Dars1(D367Y) Model Recapitulates Key Aspects of the Leukodystrophy HBSL

Hypomyelination with brain stem and spinal cord involvement and leg spasticity (HBSL) is a leukodystrophy caused by missense mutations of the aspartyl-tRNA synthetase-encoding gene DARS1. The clinical picture includes the regression of acquired motor milestones, spasticity, ataxia, seizures, nystagm...

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Autores principales: Fröhlich, Dominik, Mendes, Marisa I., Kueh, Andrew J., Bongers, Andre, Herold, Marco J., Salomons, Gajja S., Housley, Gary D., Klugmann, Matthias
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Cellular Neuroscience
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7855723/
https://www.ncbi.nlm.nih.gov/pubmed/33551752
http://dx.doi.org/10.3389/fncel.2020.625879
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author Fröhlich, Dominik
Mendes, Marisa I.
Kueh, Andrew J.
Bongers, Andre
Herold, Marco J.
Salomons, Gajja S.
Housley, Gary D.
Klugmann, Matthias
author_facet Fröhlich, Dominik
Mendes, Marisa I.
Kueh, Andrew J.
Bongers, Andre
Herold, Marco J.
Salomons, Gajja S.
Housley, Gary D.
Klugmann, Matthias
author_sort Fröhlich, Dominik
collection PubMed
description Hypomyelination with brain stem and spinal cord involvement and leg spasticity (HBSL) is a leukodystrophy caused by missense mutations of the aspartyl-tRNA synthetase-encoding gene DARS1. The clinical picture includes the regression of acquired motor milestones, spasticity, ataxia, seizures, nystagmus, and intellectual disabilities. Morphologically, HBSL is characterized by a distinct pattern of hypomyelination in the central nervous system including the anterior brainstem, the cerebellar peduncles and the supratentorial white matter as well as the dorsal columns and the lateral corticospinal tracts of the spinal cord. Adequate HBSL animal models are lacking. Dars1 knockout mice are embryonic lethal precluding examination of the etiology. To address this, we introduced the HBSL-causing Dars1(D367Y) point mutation into the mouse genome. Surprisingly, mice carrying this mutation homozygously were phenotypically normal. As hypomorphic mutations are more severe in trans to a deletion, we crossed Dars1(D367Y/D367Y) mice with Dars1-null carriers. The resulting Dars1(D367Y/−) offspring displayed a strong developmental delay compared to control Dars1(D367Y/+) littermates, starting during embryogenesis. Only a small fraction of Dars1(D367Y/−) mice were born, and half of these mice died with hydrocephalus during the first 3 weeks of life. Of the few Dars1(D367Y/−) mice that were born at term, 25% displayed microphthalmia. Throughout postnatal life, Dars1(D367Y/−) mice remained smaller and lighter than their Dars1(D367Y/+) littermates. Despite this early developmental deficit, once they made it through early adolescence Dars1(D367Y/−) mice were phenotypically inconspicuous for most of their adult life, until they developed late onset motor deficits as well as vacuolization and demyelination of the spinal cord white matter. Expression levels of the major myelin proteins were reduced in Dars1(D367Y/−) mice compared to controls. Taken together, Dars1(D367Y/−) mice model aspects of the clinical picture of the corresponding missense mutation in HBSL. This model will enable studies of late onset deficits, which is precluded in Dars1 knockout mice, and can be leveraged to test potential HBSL therapeutics including DARS1 gene replacement therapy.
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spelling pubmed-78557232021-02-04 A Hypomorphic Dars1(D367Y) Model Recapitulates Key Aspects of the Leukodystrophy HBSL Fröhlich, Dominik Mendes, Marisa I. Kueh, Andrew J. Bongers, Andre Herold, Marco J. Salomons, Gajja S. Housley, Gary D. Klugmann, Matthias Front Cell Neurosci Cellular Neuroscience Hypomyelination with brain stem and spinal cord involvement and leg spasticity (HBSL) is a leukodystrophy caused by missense mutations of the aspartyl-tRNA synthetase-encoding gene DARS1. The clinical picture includes the regression of acquired motor milestones, spasticity, ataxia, seizures, nystagmus, and intellectual disabilities. Morphologically, HBSL is characterized by a distinct pattern of hypomyelination in the central nervous system including the anterior brainstem, the cerebellar peduncles and the supratentorial white matter as well as the dorsal columns and the lateral corticospinal tracts of the spinal cord. Adequate HBSL animal models are lacking. Dars1 knockout mice are embryonic lethal precluding examination of the etiology. To address this, we introduced the HBSL-causing Dars1(D367Y) point mutation into the mouse genome. Surprisingly, mice carrying this mutation homozygously were phenotypically normal. As hypomorphic mutations are more severe in trans to a deletion, we crossed Dars1(D367Y/D367Y) mice with Dars1-null carriers. The resulting Dars1(D367Y/−) offspring displayed a strong developmental delay compared to control Dars1(D367Y/+) littermates, starting during embryogenesis. Only a small fraction of Dars1(D367Y/−) mice were born, and half of these mice died with hydrocephalus during the first 3 weeks of life. Of the few Dars1(D367Y/−) mice that were born at term, 25% displayed microphthalmia. Throughout postnatal life, Dars1(D367Y/−) mice remained smaller and lighter than their Dars1(D367Y/+) littermates. Despite this early developmental deficit, once they made it through early adolescence Dars1(D367Y/−) mice were phenotypically inconspicuous for most of their adult life, until they developed late onset motor deficits as well as vacuolization and demyelination of the spinal cord white matter. Expression levels of the major myelin proteins were reduced in Dars1(D367Y/−) mice compared to controls. Taken together, Dars1(D367Y/−) mice model aspects of the clinical picture of the corresponding missense mutation in HBSL. This model will enable studies of late onset deficits, which is precluded in Dars1 knockout mice, and can be leveraged to test potential HBSL therapeutics including DARS1 gene replacement therapy. Frontiers Media S.A. 2021-01-20 /pmc/articles/PMC7855723/ /pubmed/33551752 http://dx.doi.org/10.3389/fncel.2020.625879 Text en Copyright © 2021 Fröhlich, Mendes, Kueh, Bongers, Herold, Salomons, Housley and Klugmann. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Cellular Neuroscience
Fröhlich, Dominik
Mendes, Marisa I.
Kueh, Andrew J.
Bongers, Andre
Herold, Marco J.
Salomons, Gajja S.
Housley, Gary D.
Klugmann, Matthias
A Hypomorphic Dars1(D367Y) Model Recapitulates Key Aspects of the Leukodystrophy HBSL
title A Hypomorphic Dars1(D367Y) Model Recapitulates Key Aspects of the Leukodystrophy HBSL
title_full A Hypomorphic Dars1(D367Y) Model Recapitulates Key Aspects of the Leukodystrophy HBSL
title_fullStr A Hypomorphic Dars1(D367Y) Model Recapitulates Key Aspects of the Leukodystrophy HBSL
title_full_unstemmed A Hypomorphic Dars1(D367Y) Model Recapitulates Key Aspects of the Leukodystrophy HBSL
title_short A Hypomorphic Dars1(D367Y) Model Recapitulates Key Aspects of the Leukodystrophy HBSL
title_sort hypomorphic dars1(d367y) model recapitulates key aspects of the leukodystrophy hbsl
topic Cellular Neuroscience
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7855723/
https://www.ncbi.nlm.nih.gov/pubmed/33551752
http://dx.doi.org/10.3389/fncel.2020.625879
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