Interleukin-10-treated dendritic cells modulate immune responses of naive and sensitized T cells in vivo.

6533b7d8fe1ef96bd126a3cc

RESEARCH PRODUCT

Interleukin-10-treated dendritic cells modulate immune responses of naive and sensitized T cells in vivo.

Claudia Szalma Joachim Saloga Alexander Enk Thomas Tüting Gabriele Müller Jürgen Knop Anke Müller Kerstin Steinbrink

subject

Ovalbumin T cell T-Lymphocytes Receptors Antigen T-Cell Dermatology Biochemistry Mice medicine Cytotoxic T cell Animals Hypersensitivity Delayed Antigen-presenting cell Molecular Biology Mice Inbred BALB C CD40 biology Follicular dendritic cells Dendritic cell Cell Biology Dendritic Cells Natural killer T cell Interleukin-10 medicine.anatomical_structure Immunology biology.protein Interleukin 12

description

Interleukin-10 is a pleiotropic cytokine known to have inhibitory effects on the accessory functions of dendritic cells. In vitro, interleukin-10 converts immature dendritic cells into tolerizing antigen- presenting cells. To assess whether interleukin-10-treated dendritic cells exert tolerizing effects in vivo, CD4+ T cells from DO11.10 ovalbumin-T cell receptor transgenic mice were transferred to syngeneic BALB/c recipients. Recipient animals were treated with ovalbumin-pulsed/unpulsed, interleukin-10-treated/untreated CD11c+ dendritic cells thereafter and ovalbumin-specific proliferation of lymph node cells was assessed by restimulation with the peptide in vitro. In prophylactic experiments, recipients received naive CD4+ DO11.10 T cells and were immunized with ovalbumin323-339 peptide in incomplete Freund's adjuvant after treatment with various subtypes of dendritic cells. Strong ovalbumin-specific proliferation was observed in animals immunized with control ovalbumin-dendritic cells. Minimal proliferation was found in mice treated with ovalbumin-pulsed, interleukin-10-treated dendritic cells. In therapeutic experiments, preactivated CD4+ DO11.10 T cells were transferred, and recipients were treated with dendritic cells as described. Ovalbumin-specific proliferation was strong in recipients treated with ovalbumin-dendritic cells. CD4+ T cell proliferation from ovalbumin-interleukin-10-dendritic cell treated animals was below background. When delayed type hypersensitivity reactions in the footpads of prophylactically or therapeutically vaccinated animals were tested, mice treated with ovalbumin-interleukin-10-dendritic cells showed no footpad swelling compared with controls. Rechallenge with the antigen in vitro and in vivo did not alter the inhibitory effect of interleukin-10-treated dendritic cells. Thus, interleukin-10-treated dendritic cells inhibit ovalbumin-specific immune responses in naive and sensitized mice.

year	journal	country	edition	language
2002-10-01	The Journal of investigative dermatology

10.1046/j.1523-1747.2002.00496.x https://pubmed.ncbi.nlm.nih.gov/12406328