Myelin Basic Protein and Myelin Basic Protein Peptides Induce the Proliferation of Schwann Cells Via Ganglioside GM1 and the FGF Receptor |
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| Authors: | Tzeng Shun-Fen Deibler Gladys E. DeVries George H. |
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| Affiliation: | (1) Research Service, Hines/VA Hospital, Hines, Illinois, 60141;(2) Present address: Department of Medical Research and Education, Taichung VA Hospital, Taichung, Taiwan, Republic of China;(3) Laboratory of Cerebral Metabolism, NIMH-NIH, Bethesda, MD, 20892;(4) Department of Cell Biology, Neurobiology and Anatomy, Stritch School of Medicine-Loyola University Chicago, Maywood, Illinois, 60153 |
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| Abstract: | Myelin basic protein (MBP) and two peptides derived from MBP (MBP1–44 and MBP152–167) stimulated Schwann cell (SC) proliferation in a cAMP-mediated process. The two mitogenic regions of MBP did not compete with one another for binding to SC suggesting a distinctive SC receptor for each mitogenic peptide. Neutralizing antibodies to the fibroblast growth factor receptor blocked the mitogenic effect of the myelin-related SC mitogen found in the supernatant of myelin-fed macrophages. The binding of 125I-MBP to Schwann cells was specifically inhibited by basic fibroblast growth factor (bFGF) and conversely the binding of 125I-bFGF was competitively inhibited by MBP. These data suggested that the mitogenic effect of one MBP peptide was mediated by a bFGF receptor. The binding of MBP to ganglioside GM1 and the ability of MBP peptides containing homology to the B subunit of cholera toxin (which binds ganglioside GM1) to compete for the binding of a mitogenic peptide (MBP1–44) to SC, identified ganglioside GM1 as a second SC receptor. Based on these results, we conclude that MBP1–44 and MBP152–167 associate with ganglioside GM1 and the bFGF receptor respectively to stimulate SC mitosis. |
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| Keywords: | Myelin basic protein mitogens Schwann cell ganglioside |
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