Genetic tagging shows increased frequency and longevity of antigen-presenting, skin-derived dendritic cells in vivo
S Garg, A Oran, J Wajchman, S Sasaki, CH Maris… - Nature …, 2003 - nature.com
S Garg, A Oran, J Wajchman, S Sasaki, CH Maris, JA Kapp, J Jacob
Nature immunology, 2003•nature.comDendritic cells (DCs) are key regulators of immune responses that activate naive antigen-
specific T lymphocytes. In draining lymph nodes, antigen-bearing DCs are reported to be
rare and short-lived. How such small numbers of short-lived DCs can activate rare antigen-
specific T cells is unclear. Here we show that after immunization of mouse skins by gene
gun, the number of antigen-bearing DCs that migrate to draining lymph node is 100-fold
higher than previously estimated and that they persist for approximately 2 weeks. The …
specific T lymphocytes. In draining lymph nodes, antigen-bearing DCs are reported to be
rare and short-lived. How such small numbers of short-lived DCs can activate rare antigen-
specific T cells is unclear. Here we show that after immunization of mouse skins by gene
gun, the number of antigen-bearing DCs that migrate to draining lymph node is 100-fold
higher than previously estimated and that they persist for approximately 2 weeks. The …
Abstract
Dendritic cells (DCs) are key regulators of immune responses that activate naive antigen-specific T lymphocytes. In draining lymph nodes, antigen-bearing DCs are reported to be rare and short-lived. How such small numbers of short-lived DCs can activate rare antigen-specific T cells is unclear. Here we show that after immunization of mouse skins by gene gun, the number of antigen-bearing DCs that migrate to draining lymph node is 100-fold higher than previously estimated and that they persist for approximately 2 weeks. The substantial frequency and longevity of DCs in situ ensures ample antigen presentation and stimulation for the rare antigen-specific T cells in draining lymph nodes.
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