Occupancy of an adhesive glycoprotein receptor modulates expression of an antigenic site involved in cell adhesion.

  1. A L Frelinger, 3rd,
  2. S C Lam,
  3. E F Plow,
  4. M A Smith,
  5. J C Loftus and
  6. M H Ginsberg
  1. Department of Immunology, Research Institute of Scripps Clinic, La Jolla, California 92037.

    Abstract

    Binding of ligands that contain Arg-Gly-Asp to adhesion receptors induces cell spreading and aggregation and alters gene expression, possibly due to conformational changes within occupied adhesion receptors. PMI-1 is a monoclonal antibody which reacts with the platelet fibrinogen receptor, glycoprotein IIb-IIIa, and reports such a conformational change. ADP stimulation of platelets results in a fibrinogen-dependent increase in binding of the PMI-1 antibody. Peptides containing Arg-Gly-Asp also reversibly increase the binding of this antibody to cells and to purified glycoprotein IIb-IIIa. The PMI-1 antibody inhibits platelet adhesion and spreading on certain substrata (Shadle, P. J., Ginsberg, M. H., Plow, E. F., and Barondes, S. H. (1984) J. Cell Biol. 99, 2056-2060); thus this occupancy-modulated site may participate in adhesive function.

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    1. September 5, 1988 The Journal of Biological Chemistry, 263, 12397-12402.
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