An essential role for CD44 variant isoforms in epidermal Langerhans cell and blood dendritic cell function

JM Weiss, J Sleeman, AC Renkl, H Dittmar… - The Journal of cell …, 1997 - rupress.org
JM Weiss, J Sleeman, AC Renkl, H Dittmar, CC Termeer, S Taxis, N Howells, M Hofmann
The Journal of cell biology, 1997rupress.org
Upon antigen contact, epidermal Langerhans cells (LC) and dendritic cells (DC) leave
peripheral organs and home to lymph nodes via the afferent lymphatic vessels and then
assemble in the paracortical T cell zone and present antigen to T lymphocytes. Since splice
variants of CD44 promote metastasis of certain tumors to lymph nodes, we explored the
expression of CD44 proteins on migrating LC and DC. We show that upon antigen contact,
LC and DC upregulate pan CD44 epitopes and epitopes encoded by variant exons v4, v5 …
Upon antigen contact, epidermal Langerhans cells (LC) and dendritic cells (DC) leave peripheral organs and home to lymph nodes via the afferent lymphatic vessels and then assemble in the paracortical T cell zone and present antigen to T lymphocytes. Since splice variants of CD44 promote metastasis of certain tumors to lymph nodes, we explored the expression of CD44 proteins on migrating LC and DC. We show that upon antigen contact, LC and DC upregulate pan CD44 epitopes and epitopes encoded by variant exons v4, v5, v6, and v9. Antibodies against CD44 epitopes inhibit the emigration of LC from the epidermis, prevent binding of activated LC and DC to the T cell zones of lymph nodes, and severely inhibit their capacity to induce a delayed type hypersensitivity reaction to a skin hapten in vivo. Our results demonstrate that CD44 splice variant expression is obligatory for the migration and function of LC and DC.
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