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Enhanced Immune Response in Immunodeficient Mice Improves Peripheral Nerve Regeneration Following Axotomy

Injuries to peripheral nerves cause loss of motor and sensory function, greatly affecting life quality. Successful repair of the lesioned nerve requires efficient cell debris removal, followed by axon regeneration and reinnervation of target organs. Such process is orchestrated by several cellular a...

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Autores principales: Bombeiro, André L., Santini, Júlio C., Thomé, Rodolfo, Ferreira, Elisângela R. L., Nunes, Sérgio L. O., Moreira, Bárbara M., Bonet, Ivan J. M., Sartori, Cesar R., Verinaud, Liana, Oliveira, Alexandre L. R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4905955/
https://www.ncbi.nlm.nih.gov/pubmed/27378849
http://dx.doi.org/10.3389/fncel.2016.00151
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author Bombeiro, André L.
Santini, Júlio C.
Thomé, Rodolfo
Ferreira, Elisângela R. L.
Nunes, Sérgio L. O.
Moreira, Bárbara M.
Bonet, Ivan J. M.
Sartori, Cesar R.
Verinaud, Liana
Oliveira, Alexandre L. R.
author_facet Bombeiro, André L.
Santini, Júlio C.
Thomé, Rodolfo
Ferreira, Elisângela R. L.
Nunes, Sérgio L. O.
Moreira, Bárbara M.
Bonet, Ivan J. M.
Sartori, Cesar R.
Verinaud, Liana
Oliveira, Alexandre L. R.
author_sort Bombeiro, André L.
collection PubMed
description Injuries to peripheral nerves cause loss of motor and sensory function, greatly affecting life quality. Successful repair of the lesioned nerve requires efficient cell debris removal, followed by axon regeneration and reinnervation of target organs. Such process is orchestrated by several cellular and molecular events in which glial and immune cells actively participate. It is known that tissue clearance is largely improved by macrophages, which activation is potentiated by cells and molecules of the acquired immune system, such as T helper lymphocytes and antibodies, respectively. In the present work, we evaluated the contribution of lymphocytes in the regenerative process of crushed sciatic nerves of immunocompetent (wild-type, WT) and T and B-deficient (RAG-KO) mice. In Knockout animals, we found increased amount of macrophages under basal conditions and during the initial phase of the regenerative process, that was evaluated at 2, 4, and 8 weeks after lesion (wal). That parallels with faster axonal regeneration evidenced by the quantification of neurofilament and a growth associated protein immunolabeling. The motor function, evaluated by the sciatic function index, was fully recovered in both mouse strains within 4 wal, either in a progressive fashion, as observed for RAG-KO mice, or presenting a subtle regression, as seen in WT mice between 2 and 3 wal. Interestingly, boosting the immune response by early adoptive transference of activated WT lymphocytes at 3 days after lesion improved motor recovery in WT and RAG-KO mice, which was not ameliorated when cells were transferred at 2 wal. When monitoring lymphocytes by in vivo imaging, in both mouse strains, cells migrated to the lesion site shortly after transference, remaining in the injured limb up to its complete motor recovery. Moreover, a first peak of hyperalgesia, determined by von-Frey test, was coincident with increased lymphocyte infiltration in the damaged paw. Overall, the present results suggest that a wave of immune cell infiltration takes place during subacute phase of axonal regeneration, resulting in transient set back of motor recovery following peripheral axonal injury. Moreover, modulation of the immune response can be an efficient approach to speed up nerve regeneration.
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spelling pubmed-49059552016-07-04 Enhanced Immune Response in Immunodeficient Mice Improves Peripheral Nerve Regeneration Following Axotomy Bombeiro, André L. Santini, Júlio C. Thomé, Rodolfo Ferreira, Elisângela R. L. Nunes, Sérgio L. O. Moreira, Bárbara M. Bonet, Ivan J. M. Sartori, Cesar R. Verinaud, Liana Oliveira, Alexandre L. R. Front Cell Neurosci Neuroscience Injuries to peripheral nerves cause loss of motor and sensory function, greatly affecting life quality. Successful repair of the lesioned nerve requires efficient cell debris removal, followed by axon regeneration and reinnervation of target organs. Such process is orchestrated by several cellular and molecular events in which glial and immune cells actively participate. It is known that tissue clearance is largely improved by macrophages, which activation is potentiated by cells and molecules of the acquired immune system, such as T helper lymphocytes and antibodies, respectively. In the present work, we evaluated the contribution of lymphocytes in the regenerative process of crushed sciatic nerves of immunocompetent (wild-type, WT) and T and B-deficient (RAG-KO) mice. In Knockout animals, we found increased amount of macrophages under basal conditions and during the initial phase of the regenerative process, that was evaluated at 2, 4, and 8 weeks after lesion (wal). That parallels with faster axonal regeneration evidenced by the quantification of neurofilament and a growth associated protein immunolabeling. The motor function, evaluated by the sciatic function index, was fully recovered in both mouse strains within 4 wal, either in a progressive fashion, as observed for RAG-KO mice, or presenting a subtle regression, as seen in WT mice between 2 and 3 wal. Interestingly, boosting the immune response by early adoptive transference of activated WT lymphocytes at 3 days after lesion improved motor recovery in WT and RAG-KO mice, which was not ameliorated when cells were transferred at 2 wal. When monitoring lymphocytes by in vivo imaging, in both mouse strains, cells migrated to the lesion site shortly after transference, remaining in the injured limb up to its complete motor recovery. Moreover, a first peak of hyperalgesia, determined by von-Frey test, was coincident with increased lymphocyte infiltration in the damaged paw. Overall, the present results suggest that a wave of immune cell infiltration takes place during subacute phase of axonal regeneration, resulting in transient set back of motor recovery following peripheral axonal injury. Moreover, modulation of the immune response can be an efficient approach to speed up nerve regeneration. Frontiers Media S.A. 2016-06-14 /pmc/articles/PMC4905955/ /pubmed/27378849 http://dx.doi.org/10.3389/fncel.2016.00151 Text en Copyright © 2016 Bombeiro, Santini, Thomé, Ferreira, Nunes, Moreira, Bonet, Sartori, Verinaud and Oliveira. 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) or licensor 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 Neuroscience
Bombeiro, André L.
Santini, Júlio C.
Thomé, Rodolfo
Ferreira, Elisângela R. L.
Nunes, Sérgio L. O.
Moreira, Bárbara M.
Bonet, Ivan J. M.
Sartori, Cesar R.
Verinaud, Liana
Oliveira, Alexandre L. R.
Enhanced Immune Response in Immunodeficient Mice Improves Peripheral Nerve Regeneration Following Axotomy
title Enhanced Immune Response in Immunodeficient Mice Improves Peripheral Nerve Regeneration Following Axotomy
title_full Enhanced Immune Response in Immunodeficient Mice Improves Peripheral Nerve Regeneration Following Axotomy
title_fullStr Enhanced Immune Response in Immunodeficient Mice Improves Peripheral Nerve Regeneration Following Axotomy
title_full_unstemmed Enhanced Immune Response in Immunodeficient Mice Improves Peripheral Nerve Regeneration Following Axotomy
title_short Enhanced Immune Response in Immunodeficient Mice Improves Peripheral Nerve Regeneration Following Axotomy
title_sort enhanced immune response in immunodeficient mice improves peripheral nerve regeneration following axotomy
topic Neuroscience
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4905955/
https://www.ncbi.nlm.nih.gov/pubmed/27378849
http://dx.doi.org/10.3389/fncel.2016.00151
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