Cross-Priming of Naive Cd8 T Cells against Melanoma Antigens Using Dendritic Cells Loaded with Killed Allogeneic Melanoma Cells

Bérard, Frédéric; Blanco, Patrick; Davoust, Jean; Neidhart-Berard, Eve-Marie; Nouri-Shirazi, Mahyar; Taquet, Nicolas; Rimoldi, Donata; Cerottini, Jean Charles; Banchereau, Jacques; Palucka, A. Karolina

doi:10.1084/jem.192.11.1535

Cited by 249 publications

(166 citation statements)

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“…In the present study we found that DCs phagocytosing apoptotic tumor cells elicit long-lived combined CD4 ϩ and CD8 ϩ immunity against the poorly immunogenic B16 melanoma. DCApo have been shown by Berard et al (22) to be able to prime naive human T cells in vitro to melanoma Ags. These findings together with our preclinical model set the stage for comparable studies in humans with DC-Apo as adjuvants for active immunization against cancer.…”

Section: Discussionmentioning

confidence: 99%

“…DCs are proving to be effective in initiating and expanding immune responses in humans (10,11), providing a rationale for their use as adjuvants for active immunization against melanoma (12)(13)(14)(15)(16). Different strategies have been developed to load DCs with tumor Ags, including MHC-restricted synthetic peptides derived from the Ag (12)(13)(14)(15)(16)(17), tumor RNA (18,19), tumor lysates (20), tumor-derived exosomes (21), and dying tumor cells (22)(23)(24)(25)(26); these have been assessed in preclinical models and, in some cases, clinical trials (12)(13)(14)(15)(16)(17)(18)(19)(20)(21)(22)(23)(24)(25)(26). Tumor cells (dying cells or Ab-coated tumor cells) are of interest as an antigenic source, because the DCs would have the potential to present a broad range of tumor-associated Ags and on both MHC class I and II products regardless of the MHC haplotype of the patient (27)(28)(29)(30).…”

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Dendritic Cells Charged with Apoptotic Tumor Cells Induce Long-Lived Protective CD4+ and CD8+ T Cell Immunity against B16 Melanoma

Goldszmid

Idoyaga

Bravo³

et al. 2003

The Journal of Immunology

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Dendritic cells (DCs) are potent APCs and attractive vectors for cancer immunotherapy. Using the B16 melanoma, a poorly immunogenic experimental tumor that expresses low levels of MHC class I products, we investigated whether DCs loaded ex vivo with apoptotic tumor cells could elicit combined CD4+ and CD8+ T cell dependent, long term immunity following injection into mice. The bone marrow-derived DCs underwent maturation during overnight coculture with apoptotic melanoma cells. Following injection, DCs migrated to the draining lymph nodes comparably to control DCs at a level corresponding to ∼0.5% of the injected inoculum. Mice vaccinated with tumor-loaded DCs were protected against an intracutaneous challenge with B16, with 80% of the mice remaining tumor-free 12 wk after challenge. CD4+ and CD8+ T cells were efficiently primed in vaccinated animals, as evidenced by IFN-γ secretion after in vitro stimulation with DCs loaded with apoptotic B16 or DCs pulsed with the naturally expressed melanoma Ag, tyrosinase-related protein 2. In addition, B16 melanoma cells were recognized by immune CD8+ T cells in vitro, and cytolytic activity against tyrosinase-related protein 2180–188-pulsed target cells was observed in vivo. When either CD4+ or CD8+ T cells were depleted at the time of challenge, the protection was completely abrogated. Mice receiving a tumor challenge 10 wk after vaccination were also protected, consistent with the induction of tumor-specific memory. Therefore, DCs loaded with cells undergoing apoptotic death can prime melanoma-specific helper and CTLs and provide long term protection against a poorly immunogenic tumor in mice.

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Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

Dendritic Cells Charged with Apoptotic Tumor Cells Induce Long-Lived Protective CD4+ and CD8+ T Cell Immunity against B16 Melanoma

Goldszmid

Idoyaga

Bravo³

et al. 2003

The Journal of Immunology

177

143

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“…DCs loaded with protein can promote cellular immunity both in experimental animal models and humans (8)(9)(10)(11). Optimal antigen loading strategies provide epitopes presented by both MHC class I and class II leading to a diverse immune response in which many clones of cytotoxic T cells (CTLs) and CD4 + T cells are involved (12)(13)(14).…”

Section: Introductionmentioning

confidence: 99%

Potent Dendritic Cell Vaccine Loaded with Latent Membrane Protein 2A (LMP2A)

et al. 2008

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“…The molecular requirements for the cross-presentation of exogenous antigens by DC were also extensively analyzed in the last few years [27][28][29][30][31][32][33][34]. Because most studies analyzing cross-presentation in human DC used apoptotic cells or vesicles as the source of antigen [35,36], mechanistic analyses are not fully conclusive. Purified proteins or peptides, however, have also been used in a few studies that provided some insights into the mechanisms required for antigen delivery, processing and presentation by human DC [15,18,19,32,37,38].…”

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Long‐lasting cross‐presentation of tumor antigen in human DC

et al. 2009

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DC cross-present exogenous antigens on MHC class I molecules, a process required for the onset of anti-tumor immune responses. In order to study the cross-presentation of tumor antigens by human DC, we compared the pathways of cross-presentation of long peptides requiring internalization and intracellular processing with the direct presentation of short peptides, which does not require intracellular processing. We found that, after brief incubations with DC, short peptides were presented to CD8 1 T cells with higher efficiencies than long peptides. After longer times of chase in the absence of peptide, however, the efficiency of presentation of the two types of peptides was reversed. After 2-3 days, DC pulsed with long peptides still activated T cells efficiently, while DC pulsed with short peptides failed to do so. Long-lasting presentation of the long peptides was, at least in part, due to a stored persistent pool of antigen, which was still available for loading on MHC class I molecules after several days of chase. These results show that the use of long synthetic peptides allows the efficient, long-lasting, presentation of tumor antigens, suggesting that long peptides represent an interesting approach for active anti-tumor vaccination.Key words: Cross-presentation . CTL . DC . Long peptides . Melanoma-associated antigen Supporting Information available online IntroductionAdaptative immune responses, especially through CD8 1 T cells, can induce the rejection of solid tumors [1][2][3]. Endogenously expressed tumor-associated antigens (TAA) expressed in tumor cells are recognized by CTL through cognate interactions of the TCR with class I MHC molecules associated with 8-10 amino acid long antigenic peptides. These tumor cell/T-cell interactions, however, are not sufficient to activate naïve T lymphocytes and to induce a memory response. Indeed, professional APC are required for the induction of effector and memory tumor-specific immune responses [4,5]. As most often APC do not endogenously express TAA, uptake and presentation of antigen via an exogenous pathway is required. This so-called ''cross-presentation'' pathway is mainly performed by DC [6,7]. Following the initial observations of cross-priming of T cells by bone-marrowderived cells [8,9], numerous studies investigated the role of cross-priming in the induction of anti-tumor immune responses [10][11][12][13][14] and the strategies to manipulate cross-priming to induce and amplify tumor-specific immune responses [15][16][17][18][19]. Because 380they display a unique capacity to efficiently cross-present exogenous antigens and to prime naïve CD8 1 T cells, DC are good candidates for cancer immunotherapy. The DC-based cancer vaccines that have been tested successfully in mouse models include DC loaded with different forms of tumor antigens, including short peptides, tumor extracts, tumor-derived membrane vesicles and tumor-derived RNA [20][21][22][23]. Nevertheless, these cell-based vaccines present some disadvantages, mainly related to their cost and the...

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Cross-Priming of Naive Cd8 T Cells against Melanoma Antigens Using Dendritic Cells Loaded with Killed Allogeneic Melanoma Cells

Cited by 249 publications

References 38 publications

Dendritic Cells Charged with Apoptotic Tumor Cells Induce Long-Lived Protective CD4+ and CD8+ T Cell Immunity against B16 Melanoma

Dendritic Cells Charged with Apoptotic Tumor Cells Induce Long-Lived Protective CD4+ and CD8+ T Cell Immunity against B16 Melanoma

Potent Dendritic Cell Vaccine Loaded with Latent Membrane Protein 2A (LMP2A)

Long‐lasting cross‐presentation of tumor antigen in human DC

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