Therapeutic Cancer Vaccination with Ex Vivo RNA-Transfected Dendritic Cells—An Update

Dörrie, Jan; Schaft, Niels; Schuler, Gerold; Schuler‐Thurner, Beatrice

doi:10.3390/pharmaceutics12020092

Cited by 51 publications

(57 citation statements)

References 140 publications

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“…A fundamental breakthrough was the discovery that monocytes can be differentiated in the presence of granulocyte-macrophage colony stimulating factor (GM-CSF) and IL-4 ex vivo to moDCs at high numbers making DCs accessible for immunotherapeutic approaches [ 17 , 18 , 631 , 632 , 633 ]. To allow for the induction of immune responses, maturation of moDCs is a prerequisite.…”

Section: Harnessing the Potential Of The Immune Systems’ Generals mentioning

confidence: 99%

“…To allow for the induction of immune responses, maturation of moDCs is a prerequisite. This can be achieved by different strategies including the treatment of moDCs with agonistic αCD40 antibodies, the application of TLR ligands or via usage of the classical moDCs maturation cocktail including IL-1β, IL-6, TNFα, and Prostaglandin E2 (PGE 2 ) [ 109 , 631 , 634 , 635 , 636 , 637 , 638 ]. Before adoptive transfer, moDCs can be loaded with antigen(s) of choice.…”

Section: Harnessing the Potential Of The Immune Systems’ Generals mentioning

confidence: 99%

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Harnessing the Complete Repertoire of Conventional Dendritic Cell Functions for Cancer Immunotherapy

et al. 2020

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The onset of checkpoint inhibition revolutionized the treatment of cancer. However, studies from the last decade suggested that the sole enhancement of T cell functionality might not suffice to fight malignancies in all individuals. Dendritic cells (DCs) are not only part of the innate immune system, but also generals of adaptive immunity and they orchestrate the de novo induction of tolerogenic and immunogenic T cell responses. Thus, combinatorial approaches addressing DCs and T cells in parallel represent an attractive strategy to achieve higher response rates across patients. However, this requires profound knowledge about the dynamic interplay of DCs, T cells, other immune and tumor cells. Here, we summarize the DC subsets present in mice and men and highlight conserved and divergent characteristics between different subsets and species. Thereby, we supply a resource of the molecular players involved in key functional features of DCs ranging from their sentinel function, the translation of the sensed environment at the DC:T cell interface to the resulting specialized T cell effector modules, as well as the influence of the tumor microenvironment on the DC function. As of today, mostly monocyte derived dendritic cells (moDCs) are used in autologous cell therapies after tumor antigen loading. While showing encouraging results in a fraction of patients, the overall clinical response rate is still not optimal. By disentangling the general aspects of DC biology, we provide rationales for the design of next generation DC vaccines enabling to exploit and manipulate the described pathways for the purpose of cancer immunotherapy in vivo. Finally, we discuss how DC-based vaccines might synergize with checkpoint inhibition in the treatment of malignant diseases.

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Section: Harnessing the Potential Of The Immune Systems’ Generals mentioning

confidence: 99%

Section: Harnessing the Potential Of The Immune Systems’ Generals mentioning

confidence: 99%

Harnessing the Complete Repertoire of Conventional Dendritic Cell Functions for Cancer Immunotherapy

et al. 2020

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“…All of these pathways had positive enrichment scores, indicating that the involved genes tended to be upregulated in caIKK-DCs according to our analysis. Most protein-coding genes used as indicators of DC activation and maturation (2,53,56,57) were found to be upregulated in the enriched pathways (Supplementary Table S8). The activation of NF-κB signalling led to upregulation of surface proteins that can prime T cells (e.g., CD40, CD70, CD80, and CD86), chemokines (e.g., CCL3 and CXCL10) that are necessary for T-cell migration, TNF superfamily members that can induce crosstalk between T cells and DCs (e.g., TNF, TNFRSF4, and TNFSF9), and cytokines that are responsible for stimulating proliferation and activation of T cells (e.g., CXCL8, IL6,…”

Section: Potential Mirna-gene Interactions To Improve Caikk-dcsmentioning

confidence: 99%

“…Dendritic cells (DCs) play an important role in regulating adaptive immunity by presenting antigens to T cells (1). Due to the unique function of DCs in the coordination of adaptive immune responses, they have been tested as cell-based vaccination against tumours (2). To obtain immunogenic potency ex vivo, monocyte-derived DCs need to go through a complex maturation process, in which DCs are exposed to a monocyte-conditioned medium or a cocktail of cytokines (3,4).…”

Section: Introductionmentioning

confidence: 99%

Network and systems based re-engineering of dendritic cells with non-coding RNAs for cancer immunotherapy

Lai

Dreyer

Cantone

et al. 2020

Preprint

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Dendritic cells (DCs) are professional antigen-presenting cells that induce and regulate adaptive immunity by presenting antigens to T cells. Due to their coordinative role in adaptive immune responses, DCs have been used as cell-based therapeutic vaccination against cancer. The capacity of DCs to induce a therapeutic immune response can be enhanced by re-wiring of cellular signalling pathways with microRNAs (miRNAs). Since the activation and maturation of DCs is controlled by an interconnected signalling network, we deploy an approach that combines RNA sequencing data and systems biology methods to delineate miRNA-based strategies that enhance DC-elicited immune responses.Through RNA sequencing of IKKβ-matured DCs that are currently being tested in a clinical trial on therapeutic anti-cancer vaccination, we identified 44 differentially expressed miRNAs. According to a network analysis, most of these miRNAs regulate targets that are linked to immune pathways, such as cytokine and interleukin signalling. We employed a network topology-oriented scoring model to rank the miRNAs, analysed their impact on immunogenic potency of DCs, and identified dozens of promising miRNA candidates with miR-15a and miR-16 as the top ones. The results of our analysis are incorporated in a database which constitutes a tool to identify DC-relevant miRNA-gene interactions with therapeutic potential (www.synmirapy.net/dc-optimization).

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“…In der Tat gibt es bereits einige wenige solcher Studien, allerdings noch mit bescheidenen Erfolgen [14,46]. Auf jeden Fall unterstreicht das, dass die weitere Optimierung der aktuellen DZ‐Vakzinationsprotokolle, speziell im Hinblick auf DZ‐Züchtung, Verabreichung (zum Beispiel „Targeting“ von Antigen an definierte Untergruppen von DZ [47–50]) und Formulierung der Antigene absolut notwendig ist. Dendritische Zellen werde auch in Zukunft ein wichtiger Bestandteil im (immun)therapeutischen Armamentarium gegen Krebs bleiben.…”

Section: Diskussionunclassified

Kombination von Chemotherapie und autologen, Peptid‐beladenen dendritischen Zellen bringt Überlebensvorteil bei Melanompatienten im Stadium IV

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et al. 2020

J Deutsche Derma Gesell

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Therapeutic Cancer Vaccination with Ex Vivo RNA-Transfected Dendritic Cells—An Update

Cited by 51 publications

References 140 publications

Harnessing the Complete Repertoire of Conventional Dendritic Cell Functions for Cancer Immunotherapy

Harnessing the Complete Repertoire of Conventional Dendritic Cell Functions for Cancer Immunotherapy

Network and systems based re-engineering of dendritic cells with non-coding RNAs for cancer immunotherapy

Kombination von Chemotherapie und autologen, Peptid‐beladenen dendritischen Zellen bringt Überlebensvorteil bei Melanompatienten im Stadium IV

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