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(Received for publication, April 14, 1995; and in revised form, June 26, 1995) P-selectin glycoprotein ligand-1 (PSGL-1) is the high affinity
counter-receptor for P-selectin on myeloid cells (Sako, D., Chang, X.
J., Barone, K. M., Vachino, G., White, H. M., Shaw, G., Veldman, G. M.,
Bean, K. M., Ahern, T. J., Furie, B., Cumming, D. A., and Larsen, G.
R.(1993) Cell 75, 1179-1186). Here we demonstrate that
PSGL-1 is also widely distributed on T- and B-lymphocytic tumor cell
lines, resting peripheral blood T and B cells, and on stimulated
peripheral blood T cell and intestinal intraepithelial lymphocyte (IEL)
lines. However, the majority of PSGL-1-positive resting peripheral
blood lymphocytic cells and lymphoid tumor cell lines do not display
significant P-selectin binding. In contrast, in vitro stimulated peripheral blood T cell and IEL lines avidly bind
P-selectin, and PSGL-1 is the sole high affinity counter-receptor
mediating this binding. During the course of in vitro stimulation, cell surface expression levels of PSGL-1 do not
change as P-selectin binding increases. Rather, the activities of two
glycosyltransferases reportedly involved in the production of
functional PSGL-1 in myeloid cells are substantially higher in the
stimulated T-lymphocytic lines than in resting T lymphocytes,
consistent with the hypothesis that activation-dependent
post-translational events contribute to the expression of functional
PSGL-1 on lymphocytes.
Volume 270,
Number 37,
Issue of September 15, pp. 21966-21974, 1995
©1995 by The American Society for Biochemistry and Molecular Biology, Inc.
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