A Dual Role of erbB2 in Myelination and in Expansion of the Schwann Cell Precursor Pool

doi:10.1083/jcb.148.5.1035

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© The Rockefeller University Press, 0021-9525/2000/3/1035/ $5.00
The Journal of Cell Biology, Volume 148, Number 5, March 6, 2000 1035-1046

Original Article

A Dual Role of erbB2 in Myelination and in Expansion of the Schwann Cell Precursor Pool

Alistair N. Garratt^a, Octavian Voiculescu^b, Piotr Topilko^b, Patrick Charnay^b, and Carmen Birchmeier^a
^a Max-Delbrück-Centrum for Molecular Medicine, 13125 Berlin, Germany
^b INSERM U368, École Normale Supérieure, 75230 Paris 05, France

Correspondence to: Carmen Birchmeier, Max-Delbrück-Centrum for Molecular Medicine, Robert-Rössle-Strasse 10, 13125 Berlin, Germany. Tel:49-30-9406-2403 Fax:49-30-9406-3765 E-mail:cbirch{at}mdc-berlin.de.

Neuregulin-1 provides an important axonally derived signal forthe survival and growth of developing Schwann cells, which istransmitted by the ErbB2/ErbB3 receptor tyrosine kinases. Nullmutations of the neuregulin-1, erbB2, or erbB3 mouse genes causesevere deficits in early Schwann cell development. Here, weemploy Cre-loxP technology to introduce erbB2 mutations latein Schwann cell development, using a Krox20-cre allele. Cre-mediatederbB2 ablation occurs perinatally in peripheral nerves, butalready at E11 within spinal roots. The mutant mice exhibita widespread peripheral neuropathy characterized by abnormallythin myelin sheaths, containing fewer myelin wraps. In addition,in spinal roots the Schwann cell precursor pool is not correctlyestablished. Thus, the Neuregulin signaling system functionsduring multiple stages of Schwann cell development and is essentialfor correct myelination. The thickness of the myelin sheathis determined by the axon diameter, and we suggest that trophicsignals provided by the nerve determine the number of timesa Schwann cell wraps an axon.

Key Words: cre-loxP, neuregulin, myelin, glia, neuropathy

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