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Bromelain treatment of human T cells removes CD44, CD45RA,
E2/MIC2, CD6, CD7, CD8, and Leu 8/LAM1 surface molecules and
markedly enhances CD2-mediated T cell activation
1Hale L.P., 2HaynesB.F.
1Department of Medicine, Division of Rheumatology
and Immunology
2Department of Microbiology and Immunology, Duke
University Medical Center, Durham, NC 27710
The Journal of Immunology 1992: Vol. 149, No. 12, pp. 3809-3816
356 KA (3-06-1) |
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Abbreviations used in this paper: LFA, lymphocyte function-associated
Ag; PB, peripheral blood.
Treatment of T cells with the cysteine protease bromelain has
been widely used to enhance the binding of human T cells to human
E (autologous E rosettes) and has been shown to remove surface
T cell CD44 molecules. Ligand binding to CD44 has been shown to
markedly augment T cell activation. To study the activation potential
of bromelain-treated CD44 T cells, we have compared the proliferation
of sham- and bromelain-treated normal human PBMC to mitogenic CD2
mAb. We found that bromelain not only removed T cell CD44, but
also removed the CD45RA isoform of CD45 as well as E2/MIC2, CD6,
CD7, CD8, and Leu 8/LAM1 molecules. T cell proliferation in response
to CD2 mAb was increased 325% in bromelain-treated PBMC compared
to sham-treated PBMC (p < 0.005). Reciprocal treatment experiments
using purified T cells and monocytes demonstrated that the enhancement
of T cell CD2 activation by bromelain occurred only when T cells
were treated with bromelain and was accompanied by increased adhesion
of T cells to monocytes. These data demonstrate that expression
of portions of the extracellular domains of the CD44, CD45RA, E2/MIC2,
CD6, CD7, CD8, and Leu 8/LAM1 surface molecules are not required
for CD2 activation of human T cells. Rather, the removal of these
surface molecules by bromelain is associated with enhanced T cell-monocyte
aggregation and enhanced CD2-mediated T cell activation. Taken
together with data that CD44, E2/MIC2, CD6, and CD7 mAb inhibit
CD2/lymphocyte function-associated Ag-3-mediated cellular interactions
and also augment CD2-mediated triggering of T cells, these data
suggest that members of the bromelain-sensitive group of surface
molecules may comprise a set of CD2-associated adhesion ligands
that acts in concert to modulate human T cell activation. |
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