Radiation-driven lipid accumulation and dendritic cell dysfunction in cancer

Gao, Fu; Liu, Cong; Guo, Jiaming; Sun, Weimin; Xian, Linfeng; Bai, Dongchen; Liu, Hu; Cheng, Ying; Li, Bailong; Cui, Jianguo; Zhang, Chaoxiong; Cai, Jianming

doi:10.1038/srep09613

Cited by 60 publications

(51 citation statements)

References 32 publications

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“…These DCs exhibited endoplasmic reticulum (ER) stress and robust activation of an ER stress response factor spliced X-box-binding protein 1, which induced triglyceride biosynthesis leading to abnormal lipid accumulation. Other recent studies confirmed that dysfunction of DCs in radiation-induced thymic lymphoma and mesothelioma was mainly due to lipid accumulation [78, 79] (Fig. 2).…”

Section: Dysfunction In Cancersupporting

confidence: 65%

Dendritic cells in cancer: the role revisited

Veglia

Gabrilovich

2017

Current Opinion in Immunology

358

290

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Dendritic cells (DCs) with their potent antigen presenting ability are long considered as critical factor in antitumor immunity. Despite high potential in promoting antitumor responses, tumor-associated DCs are largely defective in their functional activity and can contribute to immune suppression in cancer. In recent years existence of immune suppressive regulatory DCs in tumor microenvironment was described. Monocytic myeloid derived suppressor cells (M-MDSCs) can contribute to the pool of tumor associated DCs by differentiating to inflammatory DCs (inf-DCs), which appear to have specific phenotype and is critical component of antitumor response. Here we examine the role of inf-DCs along with other DC subsets in the regulation of immune responses in cancer. These novel data expand our view on the role of DCs in cancer and may provide new targets for immunotherapy.

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Section: Dysfunction In Cancersupporting

confidence: 65%

Dendritic cells in cancer: the role revisited

Veglia

Gabrilovich

2017

Current Opinion in Immunology

358

290

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“…Some authors demonstrate in cancer models an opposite correlation between LD induction and Ag presentation. It was observed in murine lymphoma that lipid‐enriched dendritic cells are not able to induce CD4 T cell proliferation by the reduction in the expression of co‐stimulatory molecules and in cytokine production (IL‐12, IL‐1, and IFN‐γ) . Accordingly, it was also demonstrated that lipid‐enriched dendritic cells from tumor‐bearing mice have a reduced capacity to process and present Ags to T cells, displaying a tolerogenic phenotype.…”

Section: Lds and Antigen Presentationmentioning

confidence: 99%

“…More recently, an increase in the number of LDs in dendritic cells has been described during infection by Leishmania amazonensis or Nocardia brasiliensis and cancer. 185,[195][196][197] LDs have been described to interact with several organelles and structures within cells, including phagosomes, 91 autophagosomes, and the proteasome. 12 These results suggested that these lipid-rich organelles could be involved in cellular processes related to Ag presentation and immunity.…”

Section: Lds and Antigen Presentationmentioning

confidence: 99%

“…It was observed in murine lymphoma that lipid-enriched dendritic cells are not able to induce CD4 T cell proliferation by the reduction in the expression of co-stimulatory molecules and in cytokine production (IL-12, IL-1, and IFN-). 197 Accordingly, it was also demonstrated that lipid-enriched dendritic cells from tumor-bearing mice have a reduced capacity to process and present Ags to T cells, displaying a tolerogenic phenotype. Moreover, the pharmacological inhibition of lipid metabolism reduced dendritic cells containing lipids in tumor-bearing mice and restored their capacity to stimulate T cells.…”

Section: Lds and Antigen Presentationmentioning

confidence: 99%

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Fat, fight, and beyond: The multiple roles of lipid droplets in infections and inflammation

Pereira-Dutra

Teixeira

Costa

et al. 2019

Journal of Leukocyte Biology

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Increased accumulation of cytoplasmic lipid droplets (LDs) in host nonadipose cells is commonly observed in response to numerous infectious diseases, including bacterial, parasite, and fungal infections. LDs are lipid‐enriched, dynamic organelles composed of a core of neutral lipids surrounded by a monolayer of phospholipids associated with a diverse array of proteins that are cell and stimulus regulated. Far beyond being simply a deposit of neutral lipids, LDs have come to be seen as an essential platform for various cellular processes, including metabolic regulation, cell signaling, and the immune response. LD participation in the immune response occurs as sites for compartmentalization of several immunometabolic signaling pathways, production of inflammatory lipid mediators, and regulation of antigen presentation. Infection‐driven LD biogenesis is a complexly regulated process that involves innate immune receptors, transcriptional and posttranscriptional regulation, increased lipid uptake, and new lipid synthesis. Accumulating evidence demonstrates that intracellular pathogens are able to exploit LDs as an energy source, a replication site, and/or a mechanism of immune response evasion. Nevertheless, LDs can also act in favor of the host as part of the immune and inflammatory response to pathogens. Here, we review recent findings that explored the new roles of LDs in the context of host‐pathogen interactions.

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“…DC vaccines emerged in an effort to avoid possible interference with therapeutic efficacy due to the dysfunction of endogenous DCs, which were commonly observed in cancer patients (20,21). However, it is important that the DCs used in these vaccines are presented in a 'mature' state to activate an antigen-specific immune response upon T-cell encounter.…”

Section: Discussionmentioning

confidence: 99%

Dendritic cells loaded with the lysate of tumor cells infected with Newcastle Disease Virus trigger potent anti‑tumor immunity by promoting the secretion of IFN‑γ and IL‑2 from T cells

et al. 2018

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Abstract. Dendritic cells (DCs) are professional antigenpresenting cells that are pivotal in the generation and sustainability of antitumor immune responses. Whole tumor cell lysates (TCLs) have been used as sources of tumor antigens for the development of DC vaccines. However, the clinical outcomes of the use of TCL-based DC vaccines have so far been unsatisfactory because of the weak immunogenicity of tumor cells. To improve the efficacy of TCL-based DC vaccines, viruses have been used to enhance the immunity of TCLs and to further enhance the antigen delivery and antigen-presenting ability of DCs. The aim of the present study was to improve the antigen-presenting ability of DCs and to use them to effectively activate T lymphocytes. The present study demonstrated that DCs loaded with the lysate of Newcastle Disease Virus (NDV)-infected tumor cells (NDV-TCL) have increased levels of cluster of differentiation 80 (CD80), CD86, CD83 and human leukocyte antigen-antigen D-associated expression, compared with those loaded with TCL alone. The DCs loaded with the NDV-TCL promoted T-cell proliferation and antitumor cytokine secretion from T cells. These results indicated that loading DCs with NDV-TCL could enhance the antigen-presenting ability of the DCs. On the basis of the results of the present study, we hypothesize that this method of loading DCs with NDV-TCL can be used to develop novel DC vaccines for tumor immunotherapy in the future. IntroductionDendritic cells (DCs) are the most important antigen-presenting cells in the body; DC-based cancer immunotherapy has been investigated in previous years (1-4). Additionally, the approval of the first DC vaccine, Provenge (generic name, sipuleucel-T) (5), by the US Food and Drug Administration for the treatment of prostate cancer in 2010 was a milestone in the immunotherapeutic application of DC vaccines. Whole-tumor cell lysates (TCLs) have been used as the source of tumor antigens for the development of DC vaccines; however, the clinical outcomes of TCL-based DC vaccines have been unsatisfactory owing to the weak immunogenicity of tumor cells (6). To improve the efficacy of TCL-based DC vaccines, viruses have been used to enhance the immunity of TCLs, to further enhance the antigen delivery and to increase the antigen-presenting ability of DCs (7).The Newcastle Disease Virus (NDV) is a bird RNA virus of the Paramyxovirus family. Specifically, NDV belongs to the genus Avulavirus, which does not include any known natural pathogens of humans (8). Over the last 6 decades, NDV has been tested as an anticancer agent because of its oncolytic properties. Owing to the oncolytic and immunostimulatory properties of NDV, necrotic tumor cells destroyed by the virus are phagocytosed and perceived as dangerous by antigen-presenting cells. These professional antigen-presenting cells then process tumor-associated antigens (TAA), become activated and present the processed TAA peptides to T cells for cognate interaction and the induction of an immune response. Owing to NDV's properties ...

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Radiation-driven lipid accumulation and dendritic cell dysfunction in cancer

Cited by 60 publications

References 32 publications

Dendritic cells in cancer: the role revisited

Dendritic cells in cancer: the role revisited

Fat, fight, and beyond: The multiple roles of lipid droplets in infections and inflammation

Dendritic cells loaded with the lysate of tumor cells infected with Newcastle Disease Virus trigger potent anti‑tumor immunity by promoting the secretion of IFN‑γ and IL‑2 from T cells

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