Human Neural Cell Adhesion Molecule L1 and Rat Homologue NILE Are Ligands for Integrin αvβ3

Integrin αvβ3is distinct in its capacity to recognize the sequence Arg-Gly-Asp (RGD) in many extra-cellular matrix (ECM) components. Here, we demonstrate that in addition to the recognition of ECM components, αvβ3can interact with the neural cell adhesion molecule L1-CAM; a member of the immunoglobu...

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Bibliographic Details
Published in:The Journal of cell biology 1996-02, Vol.132 (3), p.475-485
Main Authors: Anthony M. P. Montgomery, Becker, Jurgen C., Siu, Chi-Hung, Lemmon, Vance P., Cheresh, David A., Pancook, James D., Zhao, Xiaoning, Reisfeld, Ralph A.
Format: Article
Language:English
Subjects:
Cell adhesion
Cell lines
Integrins
Ligands
Ligation
Melanoma
Molecules
Neural cell adhesion molecules
Neurons
Tumors
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Summary:Integrin αvβ3is distinct in its capacity to recognize the sequence Arg-Gly-Asp (RGD) in many extra-cellular matrix (ECM) components. Here, we demonstrate that in addition to the recognition of ECM components, αvβ3can interact with the neural cell adhesion molecule L1-CAM; a member of the immunoglobulin superfamily (IgSF). M21 melanoma cells displayed significant Ca++-dependent adhesion and spreading on immunopurified rat L1 (NILE). This adhesion was found to be dependent on the expression of the αv-integrin subunit and could be significantly inhibited by an antibody to the αvβ3heterodimer. M21 cells also displayed some αvβ3-dependent adhesion and spreading on immunopurified human L1. Ligation between this ligand and αvβ3was also observed to promote significant haptotactic cell migration. To map the site of αvβ3ligation we used recombinant L1 fragments comprising the entire extracellular domain of human L1. Significant αvβ3-dependent adhesion and spreading was evident on a L1 fragment containing Ig-like domains 4, 5, and 6. Importantly, mutation of an RGD sequence present in the sixth Ig-like domain of L1 abrogated M21 cell adhesion. We conclude that αvβ3-dependent recognition of human L1 is dependent on ligation of this RGD site. Despite high levels of L1 expression the M21 melanoma cells did not display significant adhesion via a homophilic L1-L1 interaction. These data suggest that M21 melanoma cells recognize and adhere to L1 through a mechanism that is primarily heterophilic and integrin dependent. Finally, we present evidence that melanoma cells can shed and deposit L1 in occluding ECM. In this regard, αvβ3may recognize L1 in a cell-cell or cell-substrate interaction.
ISSN:0021-9525
DOI:10.1083/jcb.132.3.475