Dissection of Complex Molecular Interactions of Neurofascin with Axonin-1, F11, and Tenascin-R, Which Promote Attachment and Neurite Formation of Tectal Cells

doi:10.1083/jcb.142.4.1083

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© The Rockefeller University Press, 0021-9525/1998//1083 $5.00
The Journal of Cell Biology, Volume 142, Number 4, , 1998 1083-1093

Articles

Dissection of Complex Molecular Interactions of Neurofascin with Axonin-1, F11, and Tenascin-R, Which Promote Attachment and Neurite Formation of Tectal Cells

Hansjürgen Volkmer, Ute Zacharias, Ursel Nörenberg, and Fritz G. Rathjen

Max-Delbrück-Centrum für Molekulare Medizin, D-13122 Berlin, Germany

Neurofascin is a member of the L1 subgroup of the Ig superfamilythat promotes axon outgrowth by interactions with neuronalNgCAM-related cell adhesion molecule (NrCAM). We used a combinationof cellular binding assays and neurite outgrowth experimentsto investigate mechanisms that might modulate the interactionsof neurofascin. In addition to NrCAM, we here demonstrate thatneurofascin also binds to the extracellular matrix glycoproteintenascin-R (TN-R) and to the Ig superfamily members axonin-1and F11.

Isoforms of neurofascin that are generated by alternative splicingshow different preferences in ligand binding. While interactionsof neurofascin with F11 are only slightly modulated, bindingto axonin-1 and TN-R is strongly regulated by alternativelyspliced stretches located in the NH₂-terminal half, and bythe proline-alanine-threonine-rich segment.

In vitro neurite outgrowth and cell attachment assays on aneurofascin-Fc substrate reveal a shift of cellular receptorusage from NrCAM to axonin-1, F11, and at least one additionalprotein in the presence of TN-R, presumably due to competitionof the neurofascin– NrCAM interaction. Thereby, F11 bindsto TN-R of the neurofascin/TN-R complex, but not to neurofascin, whereas axonin-1 is not able to bind directly to the neurofascin/TN-Rcomplex as shown by competition binding assays.

In conclusion, these investigations indicate that the molecularinteractions of neurofascin are regulated at different levels,including alternative splicing and by the presence of interactingproteins.

Key Words: neurofascin • cell adhesion • axonal outgrowth • Ig superfamily • tenascin-R

Abbreviations used in this paper: ECM, extracellular matrix; FNIII, fibronectin type III; IgSF, Ig superfamily; NCAM, neural cell adhesion molecule; NgCAM, neuron-glia cell adhesion molecule; NrCAM, NgCAM-related cell adhesion molecule; PAT, proline-alanine-threonine-rich segment; TN-C, tenascin-C; TN-R, tenascin-R.

Dr. Volkmer's present address is Naturwissenschaftliches undMedizinisches Institut, Markwiesenstr. 55, D-72770 Reutlingen,Germany.

Address all correspondence to Fritz G. Rathjen, Max-Delbrück-Centrum für Molekulare Medizin, Robert-Rössle-Str. 10, 13122Berlin, Germany. Tel.: +49-30-9406-3709; Fax:+49-30-9406-3730;E-mail: rathjen@mdc- berlin.de

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