Requirement for CD44 in activated T cell extravasation into an inflammatory site

HC DeGrendele, P Estess, MH Siegelman - Science, 1997 - science.org
HC DeGrendele, P Estess, MH Siegelman
Science, 1997science.org
Leukocytes extravasate from the blood into inflammatory sites through complementary
ligand interactions between leukocytes and endothelial cells. Activation of T cells increases
their binding to hyaluronate (HA) and enables CD44-mediated primary adhesion (rolling).
This rolling could be induced in vivo in murine Vβ8+ T cells in response to specific
superantigen stimulation; it was initially found in lymph nodes, then in peripheral blood, and
finally within the peritoneum, the original inflamed site. The migration of Vβ8+ cells into the …
Leukocytes extravasate from the blood into inflammatory sites through complementary ligand interactions between leukocytes and endothelial cells. Activation of T cells increases their binding to hyaluronate (HA) and enables CD44-mediated primary adhesion (rolling). This rolling could be induced in vivo in murine Vβ8+ T cells in response to specific superantigen stimulation; it was initially found in lymph nodes, then in peripheral blood, and finally within the peritoneum, the original inflamed site. The migration of Vβ8+ cells into the peritoneal cavity was dependent on CD44 and HA, as shown by inhibition studies. Thus, CD44-HA interactions can target lymphocytes to specific extralymphoid effector sites.
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