Literature DB >> 9775980

Chronically denervated rat Schwann cells respond to GGF in vitro.

H Li1, C Wigley, S M Hall.   

Abstract

C-erbB receptor/neuregulin signalling plays a significant role in Schwann cell function. In vivo, Schwann cells up-regulate expression of c-erbB receptors in the first month after injury, but receptor expression is down-regulated with time to levels that are not detectable immunohistochemically. The inability of chronically denervated Schwann cells to respond adequately to signals derived from regenerating axons may be one reason why delayed repair of an injured peripheral nerve frequently fails. We have examined the effects of GGF on denervated Schwann cells in vitro. A modified delayed dissociation technique was used to obtain adult rat Schwann cells from the distal stumps of transected sciatic nerves which had been acutely (7 days) or chronically (2-6 month) denervated. We found that in vitro denervated Schwann cells invariably expressed p75NTR and c-erbB receptors. There was a progressive decrease in total cell yield and the percentage of cells with Schwann cell phenotype (p75NTR and/S-100 or/laminin or /GFAP or/c-erbB positive); proliferation rate; migratory potential; and expression of the cell adhesion molecules N-CAM and N-cadherin, with increasing time of denervation. Addition of GGF2 had a significant stimulatory effect upon Schwann cell proliferation and migration, and an increased proportion of Schwann cells expressed N-CAM and N-cadherin, suggesting that these responses were mediated via GGF/c-erbB signalling. Our results support the view that it may be possible to manipulate chronically denervated Schwann cells so that they become more responsive to signals derived from regrowing axons.

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Year:  1998        PMID: 9775980

Source DB:  PubMed          Journal:  Glia        ISSN: 0894-1491            Impact factor:   7.452


  10 in total

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Review 2.  Signals that determine Schwann cell identity.

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3.  Unusual radial nerve injury by a locking compression plate for humerus fracture.

Authors:  Ahmet Kinaci; Peter Kloen; Annemieke Videler; Mick Kreulen
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4.  The role of neuregulin-1 in the response to nerve injury.

Authors:  Florence R Fricker; David Lh Bennett
Journal:  Future Neurol       Date:  2011-11

5.  Neuregulin-1 beta and neuregulin-1 alpha differentially affect the migration and invasion of malignant peripheral nerve sheath tumor cells.

Authors:  Jenell M Eckert; Stephanie J Byer; Buffie J Clodfelder-Miller; Steven L Carroll
Journal:  Glia       Date:  2009-11-01       Impact factor: 7.452

6.  Expression of ATF3 and axonal outgrowth are impaired after delayed nerve repair.

Authors:  Harukazu Saito; Lars B Dahlin
Journal:  BMC Neurosci       Date:  2008-09-18       Impact factor: 3.288

7.  Neuroblastoma in dialog with its stroma: NTRK1 is a regulator of cellular cross-talk with Schwann cells.

Authors:  Kristian W Pajtler; Ellen Mahlow; Andrea Odersky; Sven Lindner; Harald Stephan; Ivo Bendix; Angelika Eggert; Alexander Schramm; Johannes H Schulte
Journal:  Oncotarget       Date:  2014-11-30

8.  STAT3 Controls the Long-Term Survival and Phenotype of Repair Schwann Cells during Nerve Regeneration.

Authors:  Cristina Benito; Catherine M Davis; Jose A Gomez-Sanchez; Mark Turmaine; Dies Meijer; Valeria Poli; Rhona Mirsky; Kristjan R Jessen
Journal:  J Neurosci       Date:  2017-03-20       Impact factor: 6.167

Review 9.  Molecular Mechanisms Involved in Schwann Cell Plasticity.

Authors:  Angélique Boerboom; Valérie Dion; Alain Chariot; Rachelle Franzen
Journal:  Front Mol Neurosci       Date:  2017-02-17       Impact factor: 5.639

10.  Effect of delayed peripheral nerve repair on nerve regeneration, Schwann cell function and target muscle recovery.

Authors:  Samuel Jonsson; Rebecca Wiberg; Aleksandra M McGrath; Lev N Novikov; Mikael Wiberg; Liudmila N Novikova; Paul J Kingham
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  10 in total

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