Enhancing DC cancer vaccine by allogeneic MHC class II expression and Treg depletion
Noriko Seishima, William Becker, Purevdorj B. Olkhanud, Hoyoung M. Maeng, Miguel A. Lopez-Lago, William V. Williams, Jay A. Berzofsky
Noriko Seishima, William Becker, Purevdorj B. Olkhanud, Hoyoung M. Maeng, Miguel A. Lopez-Lago, William V. Williams, Jay A. Berzofsky
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Research Article Immunology Oncology

Enhancing DC cancer vaccine by allogeneic MHC class II expression and Treg depletion

Abstract

We assessed the therapeutic efficacy of a semiallogeneic dendritic cell (DC) vaccine in comparison to a syngeneic one for suppression of B16-F10 and TC-1 tumors. Syngeneic bone marrow–derived DCs (BMDCs) were generated from C57BL/6J mice and semiallogeneic BMDCs with a mutation in either MHC class I or II were generated from B6.C-H2-Kbm1/ByJ or B6(C)-H2-Ab1bm12/KhEgJ mice, respectively. We demonstrated in vivo and in vitro that the MHC class II semiallogeneic BMDC vaccine had superior efficacy over the syngeneic and the MHC class I semiallogeneic BMDC vaccine, providing allogeneic CD4+ T cell help to enhance the antitumor CD8+ T cell response through allogeneic stimulation by the mutant MHC class II molecules. We discovered that this help was induced only at an early stage of tumor growth and at a later stage of tumor growth; combining our BMDC vaccine with Treg depletion enhanced tumor suppression. We demonstrated the improved efficacy of a semiallogeneic BMDC vaccine that kept tumor-peptide presentation intact on syngeneic MHC class I molecules so that mutant MHC class II could provide allogeneic help. This strategy should enable promising new DC-based cancer immunotherapies, offering an alternative to autologous DC vaccines by incorporating allogenicity as an adjuvant.

Authors

Noriko Seishima, William Becker, Purevdorj B. Olkhanud, Hoyoung M. Maeng, Miguel A. Lopez-Lago, William V. Williams, Jay A. Berzofsky

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Figure 4

E743–77 peptide–pulsed MHC class II semiallogeneic mature BMDCs expand Th1, Th2, Tfh, and Th17 cells but reduce the proportion of Tregs.

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E743–77 peptide–pulsed MHC class II semiallogeneic mature BMDCs expand T...
(AD) In vitro CD8+ or CD4+ T cell subset changes after coculture of mixtures of splenic CD8+ T cells and CD4+ T cells from TC-1 tumor–bearing mice stimulated with either the E743–77 -pulsed syngeneic WT or MHC class II semiallogeneic bm12 mBMDCs. TC-1 tumor–bearing mice were sacrificed 8–12 days after 1 × 105 TC-1 inoculation and mixtures of 2 × 105 isolated CD8+ T cells and 2 × 105 isolated CD4+ T cells were cocultured with 1 × 105 cells of indicated mBMDCs in 200 μL/well in 96-well round-bottom plates for 48 hours and subjected to flow cytometric analysis. Data are presented as the mean ± SEM and represent 2 independent experiments, n = 4–5 per group. Statistical analysis was performed using 1-way ANOVA test with post hoc Tukey’s multiple-comparison correction. *P < 0.05; **P < 0.01; ***P < 0.001; ****P < 0.0001. mBMDC, LPS-matured BMDC; SEM, standard error of mean; ANOVA, analysis of variance.