The integrin subunit beta 1B, a beta 1 isoform with a unique sequence at the cytoplasmic domain, forms heterodimers with integrin alpha chains and binds fibronectin, but it does not localize to focal adhesion sites (Balzac, F., A. Belkin, V. Koteliansky, Y. Balabanow, F. Altruda, L. Silengo, and G. Tarone. 1993. J. Cell Biol. 121:171-178). Here we analyze the functional properties of human beta 1B by expressing it in hamster CHO cells. When stimulated by specific antibodies, beta 1B does not trigger tyrosine phosphorylation of a 125-kD cytosolic protein, an intracellular signalling pathway that is activated both by the endogenous hamster or the transfected human beta 1A. Moreover, expression of beta 1B results in reduced spreading on fibronectin and laminin, but not on vitronectin. Expression of beta 1B also results in severe reduction of cell motility in the Boyden chamber assay. Reduced cell spreading and motility could not be accounted for by preferential association of beta 1B with a given integrin alpha subunit. These data, together with our previous results, indicate that beta 1B interferes with beta 1A function when expressed in CHO cells resulting in a dominant negative effect on cell adhesion and migration.
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15 October 1994
Article|
October 15 1994
Expression of beta 1B integrin isoform in CHO cells results in a dominant negative effect on cell adhesion and motility.
F Balzac,
F Balzac
Department of Genetics, Biology and Medical Chemistry, University of Torino, Italy.
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S F Retta,
S F Retta
Department of Genetics, Biology and Medical Chemistry, University of Torino, Italy.
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A Albini,
A Albini
Department of Genetics, Biology and Medical Chemistry, University of Torino, Italy.
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A Melchiorri,
A Melchiorri
Department of Genetics, Biology and Medical Chemistry, University of Torino, Italy.
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V E Koteliansky,
V E Koteliansky
Department of Genetics, Biology and Medical Chemistry, University of Torino, Italy.
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M Geuna,
M Geuna
Department of Genetics, Biology and Medical Chemistry, University of Torino, Italy.
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L Silengo,
L Silengo
Department of Genetics, Biology and Medical Chemistry, University of Torino, Italy.
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G Tarone
G Tarone
Department of Genetics, Biology and Medical Chemistry, University of Torino, Italy.
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F Balzac
Department of Genetics, Biology and Medical Chemistry, University of Torino, Italy.
S F Retta
Department of Genetics, Biology and Medical Chemistry, University of Torino, Italy.
A Albini
Department of Genetics, Biology and Medical Chemistry, University of Torino, Italy.
A Melchiorri
Department of Genetics, Biology and Medical Chemistry, University of Torino, Italy.
V E Koteliansky
Department of Genetics, Biology and Medical Chemistry, University of Torino, Italy.
M Geuna
Department of Genetics, Biology and Medical Chemistry, University of Torino, Italy.
L Silengo
Department of Genetics, Biology and Medical Chemistry, University of Torino, Italy.
G Tarone
Department of Genetics, Biology and Medical Chemistry, University of Torino, Italy.
Online ISSN: 1540-8140
Print ISSN: 0021-9525
J Cell Biol (1994) 127 (2): 557–565.
Citation
F Balzac, S F Retta, A Albini, A Melchiorri, V E Koteliansky, M Geuna, L Silengo, G Tarone; Expression of beta 1B integrin isoform in CHO cells results in a dominant negative effect on cell adhesion and motility.. J Cell Biol 15 October 1994; 127 (2): 557–565. doi: https://doi.org/10.1083/jcb.127.2.557
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