Bone Marrow Contributes Simultaneously to Different Neural Types in the Central Nervous System through Different Mechanisms of Plasticity

Bone Marrow Contributes Simultaneously to Different Neural Types in the Central Nervous System through Different Mechanisms of Plasticity

Many studies have reported the contribution of bone marrow-derived cells (BMDC) to the CNS, raising the possibility of using them as a new source to repair damaged brain tissue or restore neuronal function. This process has mainly been investigated in the cerebellum, in which a degenerative microenv...

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Main Authors: Javier S. Recio, Manuel Álvarez-Dolado, David Díaz, Fernando C. Baltanás, Marina Piquer-Gil, José R. Alonso, Eduardo Weruaga Ph.D.
Format: Article
Language:English
Published: SAGE Publishing 2011-09-01
Series:Cell Transplantation
Online Access:https://doi.org/10.3727/096368910X552826
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spelling doaj-458964b6f0d6455abdf2f33ae2b8c61d2020-11-25T03:09:35ZengSAGE PublishingCell Transplantation0963-68971555-38922011-09-012010.3727/096368910X552826Bone Marrow Contributes Simultaneously to Different Neural Types in the Central Nervous System through Different Mechanisms of PlasticityJavier S. Recio0Manuel Álvarez-Dolado1David Díaz2Fernando C. Baltanás3Marina Piquer-Gil4José R. Alonso5Eduardo Weruaga Ph.D.6 Laboratory of Neuronal Plasticity and Neurorepair, Institute for Neuroscience of Castilla y León, Universidad de Salamanca, Salamanca, Spain Laboratory of Cell Therapy for Neuropathologies, Andalucian Center for Molecular Biology and Regenerative Medicine, CABIMER, Seville, Spain Laboratory of Neuronal Plasticity and Neurorepair, Institute for Neuroscience of Castilla y León, Universidad de Salamanca, Salamanca, Spain Laboratory of Neuronal Plasticity and Neurorepair, Institute for Neuroscience of Castilla y León, Universidad de Salamanca, Salamanca, Spain Laboratory of Cell Therapy for Neuropathologies, Andalucian Center for Molecular Biology and Regenerative Medicine, CABIMER, Seville, Spain Universidad de Tarapacá en Arica, Arica, Chile Laboratory of Neuronal Plasticity and Neurorepair, Institute for Neuroscience of Castilla y León, Universidad de Salamanca, Salamanca, SpainMany studies have reported the contribution of bone marrow-derived cells (BMDC) to the CNS, raising the possibility of using them as a new source to repair damaged brain tissue or restore neuronal function. This process has mainly been investigated in the cerebellum, in which a degenerative microenvironment has been suggested to be responsible for its modulation. The present study further analyzes the contribution of BMDC to different neural types in other adult brain areas, under both physiological and neurodegenerative conditions, together with the mechanisms of plasticity involved. We grafted genetically marked green fluorescent protein/Cre bone marrow in irradiated recipients: a) the PCD ( Purkinje Cell Degeneration ) mutant mice, suffering a degeneration of specific neuronal populations at different ages, and b) their corresponding healthy controls. These mice carried the conditional lacZ reporter gene to allow the identification of cell fusion events. Our results demonstrate that BMDC mainly generate microglial cells, although to a lesser extent a clear formation of neuronal types also exists. This neuronal recruitment was not increased by the neurodegenerative processes occurring in PCD mice, where BMDC did not contribute to rescuing the degenerated neuronal populations either. However, an increase in the number of bone marrow-derived microglia was found along the life span in both experimental groups. Six weeks after transplantation more bone marrow-derived microglial cells were observed in the olfactory bulb of the PCD mice compared to the control animals, where the degeneration of mitral cells was in process. In contrast, this difference was not observed in the cerebellum, where Purkinje cell degeneration had been completed. These findings demonstrated that the degree of neurodegenerative environment can foster the recruitment of neural elements derived from bone marrow, but also provide the first evidence that BMDC can contribute simultaneously to different encephalic areas through different mechanisms of plasticity: cell fusion for Purkinje cells and differentiation for olfactory bulb interneurons.https://doi.org/10.3727/096368910X552826
collection DOAJ
language English
format Article
sources DOAJ
author Javier S. Recio
Manuel Álvarez-Dolado
David Díaz
Fernando C. Baltanás
Marina Piquer-Gil
José R. Alonso
Eduardo Weruaga Ph.D.
spellingShingle Javier S. Recio
Manuel Álvarez-Dolado
David Díaz
Fernando C. Baltanás
Marina Piquer-Gil
José R. Alonso
Eduardo Weruaga Ph.D.
Bone Marrow Contributes Simultaneously to Different Neural Types in the Central Nervous System through Different Mechanisms of Plasticity
Cell Transplantation
author_facet Javier S. Recio
Manuel Álvarez-Dolado
David Díaz
Fernando C. Baltanás
Marina Piquer-Gil
José R. Alonso
Eduardo Weruaga Ph.D.
author_sort Javier S. Recio
title Bone Marrow Contributes Simultaneously to Different Neural Types in the Central Nervous System through Different Mechanisms of Plasticity
title_short Bone Marrow Contributes Simultaneously to Different Neural Types in the Central Nervous System through Different Mechanisms of Plasticity
title_full Bone Marrow Contributes Simultaneously to Different Neural Types in the Central Nervous System through Different Mechanisms of Plasticity
title_fullStr Bone Marrow Contributes Simultaneously to Different Neural Types in the Central Nervous System through Different Mechanisms of Plasticity
title_full_unstemmed Bone Marrow Contributes Simultaneously to Different Neural Types in the Central Nervous System through Different Mechanisms of Plasticity
title_sort bone marrow contributes simultaneously to different neural types in the central nervous system through different mechanisms of plasticity
publisher SAGE Publishing
series Cell Transplantation
issn 0963-6897
1555-3892
publishDate 2011-09-01
description Many studies have reported the contribution of bone marrow-derived cells (BMDC) to the CNS, raising the possibility of using them as a new source to repair damaged brain tissue or restore neuronal function. This process has mainly been investigated in the cerebellum, in which a degenerative microenvironment has been suggested to be responsible for its modulation. The present study further analyzes the contribution of BMDC to different neural types in other adult brain areas, under both physiological and neurodegenerative conditions, together with the mechanisms of plasticity involved. We grafted genetically marked green fluorescent protein/Cre bone marrow in irradiated recipients: a) the PCD ( Purkinje Cell Degeneration ) mutant mice, suffering a degeneration of specific neuronal populations at different ages, and b) their corresponding healthy controls. These mice carried the conditional lacZ reporter gene to allow the identification of cell fusion events. Our results demonstrate that BMDC mainly generate microglial cells, although to a lesser extent a clear formation of neuronal types also exists. This neuronal recruitment was not increased by the neurodegenerative processes occurring in PCD mice, where BMDC did not contribute to rescuing the degenerated neuronal populations either. However, an increase in the number of bone marrow-derived microglia was found along the life span in both experimental groups. Six weeks after transplantation more bone marrow-derived microglial cells were observed in the olfactory bulb of the PCD mice compared to the control animals, where the degeneration of mitral cells was in process. In contrast, this difference was not observed in the cerebellum, where Purkinje cell degeneration had been completed. These findings demonstrated that the degree of neurodegenerative environment can foster the recruitment of neural elements derived from bone marrow, but also provide the first evidence that BMDC can contribute simultaneously to different encephalic areas through different mechanisms of plasticity: cell fusion for Purkinje cells and differentiation for olfactory bulb interneurons.
url https://doi.org/10.3727/096368910X552826
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