Constitutive class I-restricted exogenous presentation of self antigens in vivo.

Kurts, Christian; Heath, William R.; Carbone, Federico; Allison, Janette; Miller, J. F. A. P.; Kanazawa, Hiroshi

doi:10.1084/jem.184.3.923

Cited by 580 publications

(599 citation statements)

References 38 publications

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“…The adoptive transfer of OT-I cells into RIPmOVA mice is a useful model in which to study functional OVA-specific T-cell responses, the induction of peripheral tolerance and ways in which this tolerance may be overcome. After transfer, OT-I cells home into the pancreatic lymph nodes where cross-presentation of OVA by DC occurs, and they undergo limited proliferation and are then rapidly depleted [25]. Destruction of OVA-expressing pancreatic islet cells (and hence diabetes) only occurs if a large number (45 Â 10 6 ) of OT-I cells are transferred [26] or if the induction of tolerance can be overcome by transferring the cells with an immune adjuvant, such as poly(I:C) or LPS [27].…”

Section: Immunostimulatory Mab Can Promote Ot-i Effectors To Promote mentioning

confidence: 99%

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Optimising anti‐tumour CD8 T‐cell responses using combinations of immunomodulatory antibodies

et al. 2008

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Immunostimulatory mAb as vaccine adjuvants for the treatment of cancer hold considerable potential for boosting weak responses when used against immunogenic tumours, or in combination with various other vaccines. We now show that when administered with OVA, the combination of anti-4-1BB mAb with anti-CD40, anti-OX40 or anti-CD25 resulted in a fourfold enhancement in the antigen-specific T-cell response compared with anti-4-1BB mAb alone, with a similar enhancement in memory responses following rechallenge with OVA. Although the number of antigen-specific T-cells generated after treatment with each of the combinations was similar, marked functional differences were detected. In particular, anti-4-1BB/anti-CD25 resulted in excellent expansion of specific CD81 T cells but produced fewer IFN-c-secreting effector cells than the other combinations. Anti-4-1BB/anti-OX40 proved to be the most potent, inducing the most effective T-cell responses in the RIPmOVA diabetes model with adoptively transferred OVA-specific T cells, and, when given with a peptide vaccine, protecting mice against the poorly immunogenic B16-F10 tumour. Overall the results suggest that although these combinations of mAb look promising in terms of their therapeutic potential, further functional assays are needed to compare their effects.

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Section: Immunostimulatory Mab Can Promote Ot-i Effectors To Promote mentioning

confidence: 99%

“…RIPmOVA mice were originally generated by Professor W. Heath (Friedrich-Wilhelms-Universität, Bonn) [25] and provided for this study by Professor Chris Kurts (Friedrich-Wilhelm's University, Bonn) and were bred heterozygously and screened by PCR for OVA expression. The B16-F10 melanoma line was obtained from the ATCC.…”

Section: Animals and Cellsmentioning

confidence: 99%

Optimising anti‐tumour CD8 T‐cell responses using combinations of immunomodulatory antibodies

et al. 2008

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“…components of vaccines, on MHC class I molecules to CD8 + T cells. This process is termed crosspresentation [2,3], and, in mice, this task is most efficiently performed by conventional CD8a + (=CD24 + ) DC [4,5] (according to the Shortman classification [6]). Signal 2, i.e.…”

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confidence: 99%

CD11c: Not merely a murine DC marker, but also a useful vaccination target

Kurts

2008

Eur J Immunol

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The induction of robust CD4 + and CD8 + T cell responses is a central aim in antiviral and anticancer vaccination. To this end, dendritic cells (DC) need to capture the vaccine, process and present it on MHC class I and II molecules. The mechanisms by which DC acquire antigen predetermine the quantity and quality of the ensuing T cell activation. In this issue of the European Journal of Immunology, it is demonstrated that targeting antigen towards CD11c, an integrin expressed preferentially by murine DC, facilitates efficient CD4 + and CD8 + T cell activation. The underlying mechanisms involve efficient antigen delivery into the marginal zone and T/DC zone of the spleen. This commentary discusses these findings in the context of current knowledge on antigen presentation.

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“…43 Briefly, spleen cells were harvested and restimulated in vitro in 24-well plates by pulsing with 1 mM ova8 (SIINFEKL) peptide for 5 days. The cell culture medium was supplemented with 1% concanavalin-Astimulated rat spleen cell supernatants beginning on day 2 in culture.…”

Section: Cytotoxicity Assaymentioning

confidence: 99%

“…For tetramer staining, single-cell suspensions (approximately 5 Â 10 5 to 1 Â 10 6 cells/well of 96-well plates) were incubated for 1.5 h at 371C in 100 ml tissue culture medium with the appropriate tetramer concentration, as determined by staining of positive control ova-TCR Tg OT-1 cells. 43 After incubation with tetramers, cells were incubated with anti-CD8-APC (clone 53-6.7), anti-CD44 FITC (clone IM7; both from Pharmingen, San Diego, CA) and with biotinylated anti-I-A b antibody (clone Y3P), followed by incubation with streptavidin PE-Cy5 conjugate (Pharmingen). For tetramer analysis, at least 200 000-500 000 total events per sample were collected.…”

Section: Mhc-peptide Tetramer Analysismentioning

confidence: 99%

Vaccination with liposome–DNA complexes elicits enhanced antitumor immunity

2006

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Cationic liposomes have been shown to potentiate markedly the ability of plasmid DNA to activate innate immune responses. We reasoned therefore that liposome-DNA complexes (LDC) could be used to produce more effective plasmid DNA vaccines for cancer. To test this hypothesis, tumor-bearing mice were vaccinated with conventional plasmid DNA vaccines or with LDC vaccines encoding model tumor antigens and CD8 þ T-cell responses and antitumor activity were assessed. We found that although plasmid DNA vaccines generated large increases in antigen-specific CD8 þ T cells, they failed to elicit significant antitumor immunity. In contrast, LDC vaccines elicited large numbers of antigen-specific CD8 þ T cells and also generated significant antitumor activity against established tumors. The antitumor activity elicited by immunization with LDC vaccines was mediated primarily by CD8 þ T cells. Studies of the interaction of LDC with antigen-presenting cells found that LDC triggered dendritic cell production of interleukin-12 and interferon (IFN)-g production by natural killer cells in vivo. Activation by LDC was also accompanied by upregulation of costimulatory molecule expression. These findings suggest that by concurrently activating strong systemic innate immune responses and generating cytotoxic T-lymphocyte responses, LDC may be used to increase the effectiveness of therapeutic plasmid DNA vaccination for cancer.

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Constitutive class I-restricted exogenous presentation of self antigens in vivo.

Cited by 580 publications

References 38 publications

Optimising anti‐tumour CD8 T‐cell responses using combinations of immunomodulatory antibodies

Optimising anti‐tumour CD8 T‐cell responses using combinations of immunomodulatory antibodies

CD11c: Not merely a murine DC marker, but also a useful vaccination target

Vaccination with liposome–DNA complexes elicits enhanced antitumor immunity

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