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Originally published as MBC in Press, 10.1091/mbc.E07-09-0869 on February 13, 2008

Vol. 19, Issue 5, 1862-1872, May 2008

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Cis-Dimerization Mediates Function of Junctional Adhesion Molecule A

Eric A. Severson, Liangyong Jiang, Andrei I. Ivanov, Kenneth J. Mandell, Asma Nusrat, and Charles A. Parkos

Epithelial Pathobiology Research Unit, Department of Pathology, Emory University, Atlanta, GA 30322

Submitted September 6, 2007; Revised January 15, 2008; Accepted February 6, 2008
Monitoring Editor: M. Bishr Omary

Junctional adhesion molecule-A (JAM-A) is a transmembrane component of tight junctions that has been proposed to play a role in regulating epithelial cell adhesion and migration, yet mechanistic structure–function studies are lacking. Although biochemical and structural studies indicate that JAM-A forms cis-homodimers, the functional significance of dimerization is unclear. Here, we report the effects of cis-dimerization–defective JAM-A mutants on epithelial cell migration and adhesion. Overexpression of dimerization-defective JAM-A mutants in 293T cells inhibited cell spreading and migration across permeable filters. Similar inhibition was observed with using dimerization-blocking antibodies. Analyses of cells expressing the JAM-A dimerization-defective mutant proteins revealed diminished β1 integrin protein but not mRNA levels. Further analyses of β1 protein localization and expression after disruption of JAM-A dimerization suggested that internalization of β1 integrin precedes degradation. A functional link between JAM-A and β1 integrin was confirmed by restoration of cell migration to control levels after overexpression of β1 integrin in JAM-A dimerization-defective cells. Last, we show that the functional effects of JAM dimerization require its carboxy-terminal postsynaptic density 95/disc-large/zonula occludins-1 binding motif. These results suggest that dimerization of JAM-A regulates cell migration and adhesion through indirect mechanisms involving posttranscriptional control of β1 integrin levels.

This was published online ahead of print in MBC in Press (http://www.molbiolcell.org/cgi/doi/10.1091/mbc.E07-09-0869) on February 13, 2008.

Address correspondence to: Charles A. Parkos (cparkos{at}emory.edu)

Abbreviations used: 6163, dimerization-defective JAM-A mutant E61A/K63A; DL1, dimerization-defective JAM-A mutant with deletion of the distal most immunoglobulin-like loop; FA, focal adhesion; JAM-A, junctional adhesion molecule A; QRT-PCR, quantitative real-time reverse transcription-polymerase chain reaction analysis.






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