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A novel biologic function of serum amyloid A. Induction of T lymphocyte migration and adhesion.

L Xu, R Badolato, W J Murphy, D L Longo, M Anver, S Hale, J J Oppenheim and J M Wang
J Immunol August 1, 1995, 155 (3) 1184-1190;
L Xu
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R Badolato
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W J Murphy
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D L Longo
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M Anver
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S Hale
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J J Oppenheim
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J M Wang
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Abstract

In the course of an inflammatory response, the concentration of serum amyloid A (SAA), a hepatocyte-derived acute phase protein, increases up to 1000-fold above the normal level. Although SAA was previously thought to be immunosuppressive, we recently reported that SAA is a potent chemoattractant for monocytes and neutrophils. The present study shows that recombinant human (rh) SAA also induces directional migration of T cells in vitro. Phenotypic analyses revealed that CD4+ and CD8+ T cell subsets were equally responsive to rhSAA, whereas CD45RA cells were also not selectively attracted by rhSAA. The T cell chemotaxis induced by rhSAA was inhibited by pretreatment of cells with pertussis toxin, suggesting the interaction of rhSAA with a G-protein-coupled receptor species. T cells pretreated with an optimal concentration of SAA exhibited enhanced adherence to human umbilical cord endothelial cell monolayers. Subcutaneous administration of rhSAA into huPBL-SCID mice caused the infiltration of human T lymphocytes at the injection sites by 4 h. These results suggest that SAA may play an important role in recruiting T lymphocytes, as well as neutrophils and monocytes into inflammatory lesions.

  • Copyright © 1995 by American Association of Immunologists

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The Journal of Immunology
Vol. 155, Issue 3
1 Aug 1995
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A novel biologic function of serum amyloid A. Induction of T lymphocyte migration and adhesion.
L Xu, R Badolato, W J Murphy, D L Longo, M Anver, S Hale, J J Oppenheim, J M Wang
The Journal of Immunology August 1, 1995, 155 (3) 1184-1190;

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A novel biologic function of serum amyloid A. Induction of T lymphocyte migration and adhesion.
L Xu, R Badolato, W J Murphy, D L Longo, M Anver, S Hale, J J Oppenheim, J M Wang
The Journal of Immunology August 1, 1995, 155 (3) 1184-1190;
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