Single-Step Antigen Loading and Activation of Dendritic Cells by mRNA Electroporation for the Purpose of Therapeutic Vaccination in Melanoma Patients

Bonehill, Aude; Nuffel, Van; Corthals, Jurgen; Tuyaerts, Sandra; Heirman, Carlo; François, Violaine; Colau, Didier; Bruggen, Pierre van der; Neyns, Bart; Thielemans, Kris

doi:10.1158/1078-0432.ccr-08-2982

Cited by 145 publications

(123 citation statements)

References 29 publications

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“…Although this technique allows substantial transfection of DCs, its efficiency is still relatively low in comparison to electroporation, where over 90% of the DCs can be transfected with mRNA. Indeed, with mRNA electroporation, TriMix does result in a significant up-regulation of maturation markers and cytokine expression, as previously reported by Bonehill et al [17]. In addition, based on the results obtained in the OT-I proliferation assay and the in vivo CTL assay, it would appear that TriO sonoporation works fine to enhance the quantity of antigen-specific CD8 + T lymphocytes (i.e.…”

Section: Discussionsupporting

confidence: 71%

“…TriMix is a mixture of 3 mRNAs, encoding CD40-ligand, a constitutively active form of TLR4 and CD70 (a co-stimulatory molecule required for effective CD8 + T cell priming) [16]. Co-delivery of these 3 nucleic acid sequences was already shown to modulate the DCs' functionality, resulting in APCs that display a more mature, T cell activating phenotype [17]. Previous studies have demonstrated the superiority of TriMix over other, more conventional, maturation stimuli after intranodal injection of TAA and TriMix mRNA in tumor-bearing mice [18].…”

Section: Introductionmentioning

confidence: 99%

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The potential of antigen and TriMix sonoporation using mRNA-loaded microbubbles for ultrasound-triggered cancer immunotherapy

Dewitte

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Heirman

et al. 2014

Journal of Controlled Release

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Dendritic cell (DC)-based cancer vaccines, where the patient's own immune system is harnessed to target and destroy tumor tissue, has emerged as a potent therapeutic strategy. In the development of such DC vaccines, it is crucial to load the DCs with tumor antigens, and to simultaneously activate them to become more potent antigen-presenting cells. For this, we report on microbubbles, loaded with both antigen mRNA as well as immunomodulating TriMix mRNA, which can be used for the ultrasound-triggered transfection of DCs. In vivo experiments with in vitro sonoporated DCs, show the effective induction of antigen-specific T cells, resulting in specific lysis of antigen-expressing cells. Especially in a therapeutic setting, sonoporation with TriMix has a significant added value, resulting in a significant reduction of tumor outgrowth and a marked increase in overall survival. What is more, complete tumor regression was observed in 30% of the antigen+TriMix DC vaccinated animals, which also displayed long-term antigen-specific immunological memory. As a result, DC sonoporation using microbubbles loaded with a combination of antigen and TriMix mRNA can elicit powerful immune responses in vivo, and might serve as a potential tool for further in vivo DC vaccination applications.

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Section: Discussionsupporting

confidence: 71%

Section: Introductionmentioning

confidence: 99%

The potential of antigen and TriMix sonoporation using mRNA-loaded microbubbles for ultrasound-triggered cancer immunotherapy

Dewitte

Lint

Heirman

et al. 2014

Journal of Controlled Release

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“…Delivery of tumor-associated antigen (TAA) and TriMix mRNA to DCs, ex vivo or in situ, reprograms them to mature antigen-presenting cells (18,19). These DCs and the T cells they activate are protected from regulatory T cells (Treg; ref.…”

Section: Introductionmentioning

confidence: 99%

Intratumoral Delivery of TriMix mRNA Results in T-cell Activation by Cross-Presenting Dendritic Cells

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Renmans

Broos

et al. 2016

Cancer Immunology Research

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“…[47][48][49] The vaccine concept may be further developed by novel strategies for enhancing DC-migration and immune stimulation. [50][51][52][53][54] We currently test the clinical use of DCs generated with a 3D protocol, based on a collaboration with Prof. Schendel and collegues. 55 This protocol includes a TLR seven out of eight agonist that enhance the IL-12 secretion of the DCs and their ability to generate Th1-like responses in vitro and in mouse models.…”

Section: Discussionmentioning

confidence: 99%

Immune response and long-term clinical outcome in advanced melanoma patients vaccinated with tumor-mRNA-transfected dendritic cells

et al. 2016

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The most effective anticancer immune responses are probably directed against patient-specific neoantigens. We have developed a melanoma vaccine targeting this individual mutanome based on dendritic cells (DCs) loaded with autologous tumor-mRNA. Here, we report a phase I/II trial evaluating toxicity, immune response and clinical outcome in 31 metastatic melanoma patients. The first cohort (n D 22) received the vaccine without any adjuvant; the next cohort (n D 9) received adjuvant IL2. Each subject received four weekly intranodal or intradermal injections, followed by optional monthly vaccines. Immune response was evaluated by delayed-type hypersensitivity (DTH), T cell proliferation and cytokine assays. Data were collected for 10 y after inclusion of the last patient. No serious adverse events were detected. In the intention-to-treat-cohort, we demonstrated significantly superior survival compared to matched controls from a benchmark meta-analysis (1 y survival 43% vs. 24%, 2 y 23% vs. 6.6%). A tumorspecific immune response was demonstrated in 16/31 patients. The response rate was higher after intradermal than intranodal vaccination (80% vs. 38%). Immune responders had improved survival compared to non-responders (median 14 mo vs. 6 mo; p D 0.030), and all eight patients surviving >20 mo were immune responders. In addition to the tumor-specific response, most patients developed a response against autologous DC antigens. The cytokine profile was polyfunctional and did not follow a Th1/Th2 dichotomy. We conclude that the favorable safety profile and evidence of a possible survival benefit warrant further studies of the RNA/DC vaccine. The vaccine appears insufficient as monotherapy, but there is a strong rationale for combination with checkpoint modulators.

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Single-Step Antigen Loading and Activation of Dendritic Cells by mRNA Electroporation for the Purpose of Therapeutic Vaccination in Melanoma Patients

Cited by 145 publications

References 29 publications

The potential of antigen and TriMix sonoporation using mRNA-loaded microbubbles for ultrasound-triggered cancer immunotherapy

The potential of antigen and TriMix sonoporation using mRNA-loaded microbubbles for ultrasound-triggered cancer immunotherapy

Intratumoral Delivery of TriMix mRNA Results in T-cell Activation by Cross-Presenting Dendritic Cells

Immune response and long-term clinical outcome in advanced melanoma patients vaccinated with tumor-mRNA-transfected dendritic cells

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