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Literature DB >> 18538865

Influence of injury severity on the rate and magnitude of the T lymphocyte and neuronal response to facial nerve axotomy.

Grace K Ha¹, Shivani Parikh, Zhi Huang, John M Petitto.

Abstract

The temporal relationship between severity of peripheral axonal injury and T lymphocyte trafficking to the neuronal cell bodies of origin in the brain has been unclear. We sought to test the hypothesis that greater neuronal death induced by disparate forms of peripheral nerve injury would result in differential patterns of T cell infiltration and duration at the cell bodies of origin in the brain and that these measures would correlate with the magnitude of neuronal death over time and cumulative neuronal loss. To test this hypothesis, we compared the time course of CD3(+) T cell infiltration and neuronal death (assessed by CD11b(+) perineuronal microglial phagocytic clusters) following axonal crush versus axonal resection injuries, two extreme variations of facial nerve axotomy that result in mild versus severe neuronal loss, respectively, in the facial motor nucleus. We also quantified the number of facial motor neurons present at 49 days post-injury to determine whether differences in the levels of neuronal death between nerve crush and resection correlated with differences in cumulative neuronal loss. Between 1 and 7 days post-injury when levels of neuronal death were minimal, we found that the rate of accumulation and magnitude of the T cell response was similar following nerve crush and resection. Differences in the T cell response were apparent by 14 days post-injury when the level of neuronal death following resection was substantially greater than that seen in crush injury. For nerve resection, the peak of neuronal death at 14 days post-resection was followed by a maximal T cell response one week later at 21 days. Differences in the level of neuronal death between the two injuries across the time course tested reflected differences in cumulative neuronal loss at 49 days post-injury. Altogether, these data suggest that the trafficking of T cells to the injured FMN is dependent upon the severity of peripheral nerve injury and associated neuronal death.

Entities: Disease Gene

Mesh：

Substances：
CD3 Complex

Year: 2008 PMID： 18538865 PMCID： PMC2577374 DOI： 10.1016/j.jneuroim.2008.04.027

Source DB: PubMed Journal: J Neuroimmunol ISSN： 0165-5728 Impact factor: 3.478

21 in total

1. Exacerbation of facial motoneuron loss after facial nerve transection in severe combined immunodeficient (scid) mice.

Authors: C J Serpe; A P Kohm; C B Huppenbauer; V M Sanders; K J Jones
Journal: J Neurosci Date: 1999-06-01 Impact factor: 6.167

2. Time course and age dependence of motor neuron death following facial nerve crush injury: role of fibroblast growth factor.

Authors: K Kuzis; J D Coffin; F P Eckenstein
Journal: Exp Neurol Date: 1999-05 Impact factor: 5.330

3. Axonal reinjury reveals the survival and re-expression of regeneration-associated genes in chronically axotomized adult mouse motoneurons.

Authors: Lowell T McPhail; Karl J L Fernandes; Carmen C M Chan; Jacqueline L Vanderluit; Wolfram Tetzlaff
Journal: Exp Neurol Date: 2004-08 Impact factor: 5.330

Review 4. The facial nerve axotomy model.

Authors: Linda B Moran; Manuel B Graeber
Journal: Brain Res Brain Res Rev Date: 2004-03

5. Lymphocyte infiltration in the injured brain: role of proinflammatory cytokines.

Authors: Gennadij Raivich; Marion Bohatschek; Alexander Werner; Leonard L Jones; Matthias Galiano; Christian U A Kloss; Xing-Zu Zhu; Klaus Pfeffer; Zhi Qiang Liu
Journal: J Neurosci Res Date: 2003-06-15 Impact factor: 4.164

6. The AP-1 transcription factor c-Jun is required for efficient axonal regeneration.

Authors: Gennadij Raivich; Marion Bohatschek; Clive Da Costa; Osuke Iwata; Matthias Galiano; Maria Hristova; Abdolrahman S Nateri; Milan Makwana; Lluís Riera-Sans; David P Wolfer; Hans-Peter Lipp; Adriano Aguzzi; Erwin F Wagner; Axel Behrens
Journal: Neuron Date: 2004-07-08 Impact factor: 17.173

7. Differences in glial, synaptic and motoneuron responses in the facial nucleus of the rat brainstem following facial nerve resection and nerve suture reanastomosis.

Authors: O Guntinas-Lichius; W F Neiss; A Gunkel; E Stennert
Journal: Eur Arch Otorhinolaryngol Date: 1994 Impact factor: 2.503

8. CD4-positive T cell-mediated neuroprotection requires dual compartment antigen presentation.

Authors: Susanna C Byram; Monica J Carson; Cynthia A DeBoy; Craig J Serpe; Virginia M Sanders; Kathryn J Jones
Journal: J Neurosci Date: 2004-05-05 Impact factor: 6.167

9. Axotomy abolishes NeuN expression in facial but not rubrospinal neurons.

Authors: Lowell T McPhail; Christopher B McBride; John McGraw; John D Steeves; Wolfram Tetzlaff
Journal: Exp Neurol Date: 2004-01 Impact factor: 5.330

10. Immune surveillance in the injured nervous system: T-lymphocytes invade the axotomized mouse facial motor nucleus and aggregate around sites of neuronal degeneration.

Authors: G Raivich; L L Jones; C U Kloss; A Werner; H Neumann; G W Kreutzberg
Journal: J Neurosci Date: 1998-08-01 Impact factor: 6.167

6 in total

Influence of injury severity on the rate and magnitude of the T lymphocyte and neuronal response to facial nerve axotomy.

1. Exacerbation of facial motoneuron loss after facial nerve transection in severe combined immunodeficient (scid) mice.

2. Time course and age dependence of motor neuron death following facial nerve crush injury: role of fibroblast growth factor.

3. Axonal reinjury reveals the survival and re-expression of regeneration-associated genes in chronically axotomized adult mouse motoneurons.

Review 4. The facial nerve axotomy model.

5. Lymphocyte infiltration in the injured brain: role of proinflammatory cytokines.

6. The AP-1 transcription factor c-Jun is required for efficient axonal regeneration.

7. Differences in glial, synaptic and motoneuron responses in the facial nucleus of the rat brainstem following facial nerve resection and nerve suture reanastomosis.

8. CD4-positive T cell-mediated neuroprotection requires dual compartment antigen presentation.

9. Axotomy abolishes NeuN expression in facial but not rubrospinal neurons.

10. Immune surveillance in the injured nervous system: T-lymphocytes invade the axotomized mouse facial motor nucleus and aggregate around sites of neuronal degeneration.

1. Age and facial nerve axotomy-induced T cell trafficking: relation to microglial and motor neuron status.

2. Motor Neurons Exhibit Sustained Loss of Atrophy Reversal in Immunodeficent Mice.

3. T cell memory in the injured facial motor nucleus: relation to functional recovery following facial nerve crush.

4. Functional recovery and facial motoneuron survival are influenced by immunodeficiency in crush-axotomized mice.

5. Dexamethasone enhanced functional recovery after sciatic nerve crush injury in rats.

6. Immune cell distribution and immunoglobulin levels change following sciatic nerve injury in a rat model.