Abbreviated Exposure to Hypoxia Is Sufficient to Induce CNS Dysmyelination, Modulate Spinal Motor Neuron Composition, and Impair Motor Development in Neonatal Mice

Neonatal white matter injury (nWMI) is an increasingly common cause of cerebral palsy that results predominantly from hypoxic injury to progenitor cells including those of the oligodendrocyte lineage. Existing mouse models of nWMI utilize prolonged periods of hypoxia during the neonatal period, requ...

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Autores principales: Watzlawik, Jens O., Kahoud, Robert J., O’Toole, Ryan J., White, Katherine A. M., Ogden, Alyssa R., Painter, Meghan M., Wootla, Bharath, Papke, Louisa M., Denic, Aleksandar, Weimer, Jill M., Carey, William A., Rodriguez, Moses
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/PMC4447462/
https://www.ncbi.nlm.nih.gov/pubmed/26020269
http://dx.doi.org/10.1371/journal.pone.0128007
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author Watzlawik, Jens O.
Kahoud, Robert J.
O’Toole, Ryan J.
White, Katherine A. M.
Ogden, Alyssa R.
Painter, Meghan M.
Wootla, Bharath
Papke, Louisa M.
Denic, Aleksandar
Weimer, Jill M.
Carey, William A.
Rodriguez, Moses
author_facet Watzlawik, Jens O.
Kahoud, Robert J.
O’Toole, Ryan J.
White, Katherine A. M.
Ogden, Alyssa R.
Painter, Meghan M.
Wootla, Bharath
Papke, Louisa M.
Denic, Aleksandar
Weimer, Jill M.
Carey, William A.
Rodriguez, Moses
author_sort Watzlawik, Jens O.
collection PubMed
description Neonatal white matter injury (nWMI) is an increasingly common cause of cerebral palsy that results predominantly from hypoxic injury to progenitor cells including those of the oligodendrocyte lineage. Existing mouse models of nWMI utilize prolonged periods of hypoxia during the neonatal period, require complex cross-fostering and exhibit poor growth and high mortality rates. Abnormal CNS myelin composition serves as the major explanation for persistent neuro-motor deficits. Here we developed a simplified model of nWMI with low mortality rates and improved growth without cross-fostering. Neonatal mice are exposed to low oxygen from postnatal day (P) 3 to P7, which roughly corresponds to the period of human brain development between gestational weeks 32 and 36. CNS hypomyelination is detectable for 2–3 weeks post injury and strongly correlates with levels of body and brain weight loss. Immediately following hypoxia treatment, cell death was evident in multiple brain regions, most notably in superficial and deep cortical layers as well as the subventricular zone progenitor compartment. PDGFαR, Nkx2.2, and Olig2 positive oligodendrocyte progenitor cell were significantly reduced until postnatal day 27. In addition to CNS dysmyelination we identified a novel pathological marker for adult hypoxic animals that strongly correlates with life-long neuro-motor deficits. Mice reared under hypoxia reveal an abnormal spinal neuron composition with increased small and medium diameter axons and decreased large diameter axons in thoracic lateral and anterior funiculi. Differences were particularly pronounced in white matter motor tracts left and right of the anterior median fissure. Our findings suggest that 4 days of exposure to hypoxia are sufficient to induce experimental nWMI in CD1 mice, thus providing a model to test new therapeutics. Pathological hallmarks of this model include early cell death, decreased OPCs and hypomyelination in early postnatal life, followed by dysmyelination, abnormal spinal neuron composition, and neuro-motor deficits in adulthood.
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spelling pubmed-44474622015-06-09 Abbreviated Exposure to Hypoxia Is Sufficient to Induce CNS Dysmyelination, Modulate Spinal Motor Neuron Composition, and Impair Motor Development in Neonatal Mice Watzlawik, Jens O. Kahoud, Robert J. O’Toole, Ryan J. White, Katherine A. M. Ogden, Alyssa R. Painter, Meghan M. Wootla, Bharath Papke, Louisa M. Denic, Aleksandar Weimer, Jill M. Carey, William A. Rodriguez, Moses PLoS One Research Article Neonatal white matter injury (nWMI) is an increasingly common cause of cerebral palsy that results predominantly from hypoxic injury to progenitor cells including those of the oligodendrocyte lineage. Existing mouse models of nWMI utilize prolonged periods of hypoxia during the neonatal period, require complex cross-fostering and exhibit poor growth and high mortality rates. Abnormal CNS myelin composition serves as the major explanation for persistent neuro-motor deficits. Here we developed a simplified model of nWMI with low mortality rates and improved growth without cross-fostering. Neonatal mice are exposed to low oxygen from postnatal day (P) 3 to P7, which roughly corresponds to the period of human brain development between gestational weeks 32 and 36. CNS hypomyelination is detectable for 2–3 weeks post injury and strongly correlates with levels of body and brain weight loss. Immediately following hypoxia treatment, cell death was evident in multiple brain regions, most notably in superficial and deep cortical layers as well as the subventricular zone progenitor compartment. PDGFαR, Nkx2.2, and Olig2 positive oligodendrocyte progenitor cell were significantly reduced until postnatal day 27. In addition to CNS dysmyelination we identified a novel pathological marker for adult hypoxic animals that strongly correlates with life-long neuro-motor deficits. Mice reared under hypoxia reveal an abnormal spinal neuron composition with increased small and medium diameter axons and decreased large diameter axons in thoracic lateral and anterior funiculi. Differences were particularly pronounced in white matter motor tracts left and right of the anterior median fissure. Our findings suggest that 4 days of exposure to hypoxia are sufficient to induce experimental nWMI in CD1 mice, thus providing a model to test new therapeutics. Pathological hallmarks of this model include early cell death, decreased OPCs and hypomyelination in early postnatal life, followed by dysmyelination, abnormal spinal neuron composition, and neuro-motor deficits in adulthood. Public Library of Science 2015-05-28 /pmc/articles/PMC4447462/ /pubmed/26020269 http://dx.doi.org/10.1371/journal.pone.0128007 Text en © 2015 Watzlawik 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
Watzlawik, Jens O.
Kahoud, Robert J.
O’Toole, Ryan J.
White, Katherine A. M.
Ogden, Alyssa R.
Painter, Meghan M.
Wootla, Bharath
Papke, Louisa M.
Denic, Aleksandar
Weimer, Jill M.
Carey, William A.
Rodriguez, Moses
Abbreviated Exposure to Hypoxia Is Sufficient to Induce CNS Dysmyelination, Modulate Spinal Motor Neuron Composition, and Impair Motor Development in Neonatal Mice
title Abbreviated Exposure to Hypoxia Is Sufficient to Induce CNS Dysmyelination, Modulate Spinal Motor Neuron Composition, and Impair Motor Development in Neonatal Mice
title_full Abbreviated Exposure to Hypoxia Is Sufficient to Induce CNS Dysmyelination, Modulate Spinal Motor Neuron Composition, and Impair Motor Development in Neonatal Mice
title_fullStr Abbreviated Exposure to Hypoxia Is Sufficient to Induce CNS Dysmyelination, Modulate Spinal Motor Neuron Composition, and Impair Motor Development in Neonatal Mice
title_full_unstemmed Abbreviated Exposure to Hypoxia Is Sufficient to Induce CNS Dysmyelination, Modulate Spinal Motor Neuron Composition, and Impair Motor Development in Neonatal Mice
title_short Abbreviated Exposure to Hypoxia Is Sufficient to Induce CNS Dysmyelination, Modulate Spinal Motor Neuron Composition, and Impair Motor Development in Neonatal Mice
title_sort abbreviated exposure to hypoxia is sufficient to induce cns dysmyelination, modulate spinal motor neuron composition, and impair motor development in neonatal mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4447462/
https://www.ncbi.nlm.nih.gov/pubmed/26020269
http://dx.doi.org/10.1371/journal.pone.0128007
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