Regulation of fibronectin and laminin binding activity in cultured human lymphoblastic cell lines
- 1 March 1993
- journal article
- research article
- Published by Wiley in Journal of Cellular Physiology
- Vol. 154 (3) , 593-600
- https://doi.org/10.1002/jcp.1041540318
Abstract
The current study shows that a clonal derivative of the Jurkat cell line up-regulates both the avidity and density of the α 6/β1 receptor in response to phorbol 12-myristate 13-acetate (PMA). This derivative attaches to fibronectin and, to a lesser degree, laminin constitutively. Adhesion and spreading are dramatically up-regulated following treatment with PMA. The response on fibronectin peaks within 4 hours, is insensitive to cyclohexaminde, can be blocked by monoclonal antibodies (Mabs) to the β1 and α 5 subunits of the β1 family of integrins, and is not associated with increased expression of the α 5 or β1 epitopes at the cell surface. In contrast, the response on laminin is biphasic. The early phase parallels the response on fibronectin. The second phase peaks after 48–72 hours of treatment with PMA, is sensitive to cycloheximide, can be blocked by Mabs to the β1 and α 6 subunits, and is associated with increased expression of the α 6 epitope. Both the density independent and dependent responses to PMA in Jurkat cells are blocked by the protein kinase inhibitor staurosporine. The HSB-2, CEM, Molt-4, and HPB-ALL T-lymphoblastic cell lines also up-regulate attachment to fibronectin and laminin following treatment with PMA. All four lines constitutively attach to fibronectin and show rapid up-regulation of attachment following treatment with PMA. None of the lines attach to laminin prior to PMA treatment; however, specific adhesion developed after 4–120 hours of treatment. The most mature lines (Jurkat and HPB-ALL) up-regulated adhesion on laminin more rapidly than the less phenotypically mature lines (CEM, Molt-4, and HSB-2). In summary, clonal derivatives of the Jurkat cell line up-regulated attachment to laminin through protein kinase dependent increases in α /β1 receptor avidity and density. In addition, the expression of functional receptors for laminin is linked to developmental maturity in a series of T-lymphoblastic cell lines.Keywords
This publication has 33 references indexed in Scilit:
- T cell antigen receptor activation pathways: The tyrosine kinase connectionCell, 1991
- β1 Integrin‐mediated lymphocyte adherence to extracellular matrix is enhanced by phorbol ester treatmentEuropean Journal of Immunology, 1991
- Evidence for protein kinase C independent activation of phospholipase D by phorbol esters in lymphocytesBiochemical and Biophysical Research Communications, 1990
- Identification and characterization of the T lymphocyte adhesion receptor for an alternative cell attachment domain (CS-1) in plasma fibronectin.The Journal of cell biology, 1989
- Synthesis and expression of the fibroblast fibronectin receptor in human monocytes.Journal of Clinical Investigation, 1989
- The function of multiple extracellular matrix receptors in mediating cell adhesion to extracellular matrix: preparation of monoclonal antibodies to the fibronectin receptor that specifically inhibit cell adhesion to fibronectin and react with platelet glycoproteins Ic-IIa.The Journal of cell biology, 1988
- Differential down‐regulation of protein kinase C subspecies in KM3 cellsFEBS Letters, 1988
- Identification of fibronectin receptors on T lymphocytes.The Journal of cell biology, 1987
- Homing of hemopoietic precursor cells to the embryonic thymus: characterization of an invasive mechanism induced by chemotactic peptides.The Journal of cell biology, 1986
- Cloning and expression of multiple protein kinase C cDNAsCell, 1986