Delineation of Five Thyroglobulin T Cell Epitopes with Pathogenic Potential in Experimental Autoimmune Thyroiditis

et al. 2010

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oBJective: In NOD.H2 h4 mice, high dietary iodine intake has been known to cause Iodineaccelerated spontaneous Autoimmune thyroiditis (IsAt) via an unknown mechanism. the aim of the study was to examine whether the NOD.H2 h4 genetic background predisposes to enhanced iodine organification in thyroglobulin (tg), a target autoantigen in IsAt. DEsIGN: to avoid issues associated with an ongoing anti-tg antibody response, we assessed tg iodination levels in iodine-fed, b-cell deficient NOD.H2 h4 mice. Additionally, we tested whether humoral or cellular immune responses of iodine-fed NOD.H2 h4 mice are preferentially directed to tg with increased iodine content (I-tg) or known pathogenic tg peptides that contained iodine. rEsULts: the iodine content of tg was not significantly different between control (9.0±2.7 I atoms per monomer) and iodine-fed mice (10.9±0.3 I atoms per monomer). Furthermore, in iodine-fed NOD.H2 h4 mice developing IsAt, strong but equivalent serum IgG responses were detected to both tg or I-tg, whereas their lymphoid cells were stimulated weakly but equally well by tg or I-tg in vitro and did not show reactivity against a panel of five pathogenic tg peptides that contained iodine. cONcLUsIONs: the results suggest that development of IsAt in NOD.H2 h4 mice is not associated with enhanced iodine organification or differential b-or t-cell responses to iodinated determinants in tg.

Section: Introductioncontrasting

confidence: 53%

Iodine content of thyroglobulin in NOD.H2h4 mice developing iodine-accelerated autoimmune thyroiditis

Kolypetri

Noel

et al. 2010

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“…of outbred ICR mice (Harlan Bioproducts for Science), as previously described (25). OVA was purchased from Sigma-Aldrich.…”

Section: Tolerogenic Semimature Dendritic Cells Suppressmentioning

confidence: 99%

“…Thyroid glands were removed 18 -21 days after Tg challenge to be assessed for thyroid pathology. Fixation, embedding, and sectioning of thyroids were performed, as previously described (25). Histological sections were stained with H&E, and the mononuclear cell infiltration index (I.I.)…”

Section: Eat Inductionmentioning

confidence: 99%

“…Eighteen hours before harvesting, 1 Ci of [ 3 H]thymidine (6.7 Ci/mol; DuPont Pharmaceuticals) was added to each well in 25 l of complete medium. Cell harvesting and radioactivity measurements were performed, as previously described (25). Stimulation index is defined as: (cpm in the presence of Ag)/(cpm in the absence of Ag).…”

Section: T Cell Proliferation Assaysmentioning

confidence: 99%

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Tolerogenic Semimature Dendritic Cells Suppress Experimental Autoimmune Thyroiditis by Activation of Thyroglobulin-Specific CD4+CD25+ T Cells

Verginis

The Journal of Immunology

2005

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163

119

Ex vivo treatment of bone marrow-derived dendritic cells (DCs) with TNF-α has been previously shown to induce partial maturation of DCs that are able to suppress autoimmunity. In this study, we demonstrate that i.v. administration of TNF-α-treated, semimature DCs pulsed with thyrogloblin (Tg), but not with OVA Ag, inhibits the subsequent development of Tg-induced experimental autoimmune thyroiditis (EAT) in CBA/J mice. This protocol activates CD4+CD25+ T cells in vivo, which secrete IL-10 upon specific recognition of Tg in vitro and express regulatory T cell (Treg)-associated markers such as glucocorticoid-induced TNFR, CTLA-4, and Foxp3. These CD4+CD25+ Treg cells suppressed the proliferation and cytokine release of Tg-specific, CD4+CD25− effector cells in vitro, in an IL-10-independent, cell contact-dependent manner. Prior adoptive transfer of the same CD4+CD25+ Treg cells into CBA/J hosts suppressed Tg-induced EAT. These results demonstrate that the tolerogenic potential of Tg-pulsed, semimature DCs in EAT is likely to be mediated through the selective activation of Tg-specific CD4+CD25+ Treg cells and provide new insights for the study of Ag-specific immunoregulation of autoimmune diseases.

“…Since its discovery as an autoantigen in 1956 (13), 25 Tg pathogenic epitopes have been identified using a variety of approaches (14). A common strategy involved the use of computer algorithms to delineate putative MHC-binding Tg peptides (15)(16)(17)(18)(19), whereas other methods used cloned T cell hybridomas as screening tools (20,21), elution of human MHC-bound peptides (22,23), or focused on searching for T cell epitopes shared between Tg and thyroid peroxidase (24). All known Tg pathogenic peptides have fallen under three categories: 1) iodinated peptides containing iodotyrosyls; 2) peptides encompassing hormonogenic sites; and 3) noniodinated peptides scattered throughout the Tg molecule (14).…”

Section: E Xperimental Autoimmune Thyroiditis (Eat) a Model Ofmentioning

confidence: 99%

Identification of Pathogenic T Cell Epitopes Near Cathepsin Cleavage Sites in Thyroglobulin

Kolypetri

Jiang

The Journal of Immunology

2013

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Experimental autoimmune thyroiditis, induced in mice after challenge with thyroglobulin (Tg), is known to be under the genetic control of the H2Ak locus. Because cathepsins are known to influence proteolytic processing of Tg in vivo, we examined in this study whether putative H2Ak-binding Tg epitopes, located near cathepsin cleavage sites within mouse Tg, have immunopathogenic properties. Cathepsin L, B, and D cleavage sites in mouse Tg were predicted based on homology with known cathepsin cleavage sites in rabbit Tg. We used an algorithm-based approach to identify H2Ak-binding motifs within 20-aa residue segments adjacent to cathepsin cleavage sites, and five 12mer peptides encompassing these sequences were synthesized. Two of them, p2369 (aa 2369–2380) and p2439 (aa 2439–2450) were immunogenic, eliciting significant proliferative T cell responses using lymph node cells from peptide-primed mice and production of IL-2 and IFN-γ in recall assays in vitro. Both peptides induced experimental autoimmune thyroiditis upon direct challenge of CBA/J mice with peptide in CFA and by adoptive transfer of peptide-primed lymph node cells into naive recipient hosts, but neither peptide was characterized as dominant.