The Journal of Cell Biology, Vol 116, 177-185, Copyright © 1992 by The Rockefeller University Press

ARTICLES

Stromelysin generates a fibronectin fragment that inhibits Schwann cell proliferation

D Muir and M Manthorpe
Department of Biology, University of California, San Diego, La Jolla 92093.

Our previous report (Muir, D., S. Varon, and M. Manthorpe. 1990. J. Cell Biol. 109:2663-2672) described the isolation and partial characterization of a 55-kD antiproliferative protein found in Schwann cell (SC) and schwannoma cell line-conditioned media and we concluded that SC proliferation is under negative autocrine control. In the present study the 55-kD protein was found to possess metalloprotease activity and stromelysin immunoreactivity. The SC-derived metalloprotease shares many properties with stromelysin isolated from other sources including the ability to cleave fibronectin (FN). Furthermore, limited proteolysis of FN by the SC-derived protease generated a FN fragment which itself expresses a potent antiproliferative activity for SCs. The active FN fragment corresponds to the 29-kD amino-terminal region of the FN molecule which was also identified as an active component in SC CM. Additional evidence that a proteolytic fragment of FN can possess antiproliferative activity for SCs was provided by the finding that plasmin can generate an amino- terminal FN fragment which mimicked the activity of the SC metalloprotease-generated antiproliferative FN fragment. Both the 55-kD SC metalloprotease and the 29-kD FN fragment could completely and reversibly inhibit proliferation of SCs treated with various mitogens and both were largely ineffective at inhibiting proliferation by immortalized or transformed SC lines. Normal and transformed SC types do secrete the proform of stromelysin, however, transformed cultures do not produce activated stromelysin and thus cannot generate the antiproliferative fragment of FN. These results suggest that, once activated, a SC-derived protease similar to stromelysin cleaves FN and generates an antiproliferative activity which can maintain normal SC quiescence in vitro.
CiteULike    Complore    Connotea    Del.icio.us    Digg    Facebook    Reddit    Technorati    Twitter    What's this?

This article has been cited by other articles:

• Hall, S. (2005). The response to injury in the peripheral nervous system. J Bone Joint Surg Br 87-B: 1309-1319 [Full Text]  
• Schor, S. L., Ellis, I. R., Jones, S. J., Baillie, R., Seneviratne, K., Clausen, J., Motegi, K., Vojtesek, B., Kankova, K., Furrie, E., Sales, M. J., Schor, A. M., Kay, R. A. (2003). Migration-Stimulating Factor: A Genetically Truncated Onco-Fetal Fibronectin Isoform Expressed by Carcinoma and Tumor-Associated Stromal Cells. Cancer Res. 63: 8827-8836 [Abstract] [Full Text]  
• Fleur, M. L., Underwood, J. L., Rappolee, D. A., Werb, Z. (1996). Basement Membrane and Repair of Injury to Peripheral Nerve: Defining a Potential Role for Macrophages, Matrix Metalloproteinases, and Tissue Inhibitor of Metalloproteinases-1. JEM 184: 2311-2326 [Abstract] [Full Text]  
• Schor, S., Ellis, I, Dolman, C, Banyard, J, Humphries, M., Mosher, D., Grey, A., Mould, A., Sottile, J, Schor, A. (1996). Substratum-dependent stimulation of fibroblast migration by the gelatin-binding domain of fibronectin. J. Cell Sci. 109: 2581-2590 [Abstract]  
• Feltri, M., Scherer, S., Nemni, R, Kamholz, J, Vogelbacker, H, Scott, M., Canal, N, Quaranta, V, Wrabetz, L (1994). Beta 4 integrin expression in myelinating Schwann cells is polarized, developmentally regulated and axonally dependent. Development 120: 1287-1301 [Abstract]  

Home | Help | Feedback | Subscriptions | Archive | Search | Table of Contents