Ablation of adhesion molecule L1 in mice favours Schwann cell proliferation and functional recovery after peripheral nerve injury

doi:10.1093/brain/awp160

Brain Advance Access published online on June 18, 2009
Brain, doi:10.1093/brain/awp160

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Ablation of adhesion molecule L1 in mice favours Schwann cell proliferation and functional recovery after peripheral nerve injury

Daria Guseva¹, Doychin N. Angelov², Andrey Irintchev¹^,3 and Melitta Schachner¹^,4^,5

1 Zentrum für Molekulare Neurobiologie, Universität Hamburg, Hamburg, Germany 2 Anatomical Institute I, University of Cologne, Cologne, Germany 3 Department of Otorhinolaryngology, Friedrich-Schiller-University Jena, Jena, Germany 4 W. M. Keck Center for Collaborative Neuroscience and Department of Cell Biology and Neuroscience, Rutgers University, NJ, USA 5 Center for Neuroscience, Shantou University Medical College, Shantou, China

Correspondence to: Melitta Schachner, Zentrum für Molekulare Neurobiologie, Universität Hamburg, Martinistrasse 52, D-20246 Hamburg, Germany E-mail: melitta.schachner{at}zmnh.uni-hamburg.de Correspondence may also be addressed to: Andrey Irintchev, Department of Otorhinolaryngology, Friedrich-Schiller-University Jena, Lessingstrasse 2, D-07740 Jena, Germany E-mail: andrey.irintchev{at}med.uni-jena.de

The adhesion molecule L1 is one of the few adhesion moleculesknown to be beneficial for repair processes in the adult centralnervous system of vertebrates by promoting axonal growth andneuronal survival. In the peripheral nervous system, L1 is up-regulatedby myelination-competent Schwann cells and regenerating axonsafter nerve damage but its functional role has remained unknown.Here we tested the hypothesis that L1 is, as in the centralnervous system, beneficial for nerve regeneration in the peripheralnervous system by performing combined functional and histologicalanalyses of adult L1-deficient mice (L1y/–) and wild-type(L1y/+) littermates. Contrary to our hypothesis, quantitativevideo-based motion analysis revealed better locomotor recoveryin L1y/– than in L1y/+ mice at 4–12 weeks aftertransection and surgical repair of the femoral nerve. Motoneuronregeneration in L1y/– mice was also enhanced as indicatedby attenuated post-traumatic loss of motoneurons, enhanced precisionof motor reinnervation, larger cell bodies of regenerated motoneuronsand diminished loss of inhibitory synaptic input to motoneurons.In search of mechanisms underlying the observed effects, weanalysed peripheral nerves at short time-periods (3–14days) after transection and found that Schwann cell proliferationis strongly augmented in L1y/– versus L1y/+ mice. L1-deficientSchwann cells showed increased proliferation than wild-typeSchwann cells, both in vivo and in vitro. These findings suggesta novel role for L1 in nerve regeneration. We propose that L1negatively regulates Schwann cell proliferation after nervedamage, which in turn restricts functional recovery by limitingthe trophic support for regenerating motoneurons.

Key Words: adhesion molecule L1; femoral nerve; Schwann cells; peripheral nerve regeneration; motoneuron

Received December 14, 2008. Revised April 25, 2009. Accepted May 12, 2009.

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