Cutting edge: TLR ligands are not sufficient to break cross-tolerance to self-antigens

Hamilton-Williams, EE; Lang, A; Benke, D; Davey, GM; Wiesmuller, KH; Kurts, C

Author(s): Hamilton-Williams, EE; Lang, A; Benke, D; Davey, GM; Wiesmuller, KH; Kurts, C;
Details: Publication Year 2005-02-01,Volume 174,Issue #3,Page 1159-1163
Journal Title: JOURNAL OF IMMUNOLOGY
Publication Type: Journal Article
Abstract: Cross-presentation of peripheral self-Ags by dendritic cells (DC) can induce deletion of autoreactive CTL by a mechanism termed cross-tolerance. Activation of DC by microbial TLR ligands is thought to result in adaptive immunity. However, activation of tolerogenic DC may cause autoimmunity by stimulating instead of deleting autoreactive CTL. To investigate this scenario, we have monitored the response of autoreactive CTL in specific for the transgenic self Ag, OVA, expressed in pancreatic islets of RIP-mOVA mice injected with ligands of TLR2, 3, 4, and 9. This somewhat enhanced proliferation and cytokine production, and moderately reduced the CTL number able to induce autoimmunity. Nevertheless, physiological CTL numbers were deleted before disease ensued, unless was provided. In conclusion, DC specific CD4 T cell help activation by TLR ligands was insufficient to break peripheral cross-tolerance in the absence of specific CD4 T cell help, and triggered autoimmunity by stimulating the early effector phase of autoreactive CTL only when their precursor frequency was extremely high.
Publisher: AMER ASSOC IMMUNOLOGISTS
Keywords: TOLL-LIKE RECEPTORS; CD8 T-CELLS; DENDRITIC CELLS; IMMUNITY; INNATE; AUTOIMMUNITY; ACTIVATION; DELETION; APC; CTL
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Creation Date: 2005-02-01 12:00:00