Engineered CD8+ cytotoxic T cells with fiber-modified adenovirus-mediated TNF-α gene transfection counteract immunosuppressive interleukin-10-secreting lung metastasis and solid tumors

Ye, Z; Shi, Meiqing; Chan, Tim; Sas, S; Xu, Shuling; Xiang, Jim

doi:10.1038/sj.cgt.7701039

Cited by 11 publications

(10 citation statements)

References 61 publications

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“…TNF behaved as an immunoadjuvant through inducing major histocompatibility complex (MHC) class I molecules or maintaining DCs’ maturation status[141, 142]. Similarly, TNF gene-engineered CD8+ cytotoxic T cells had enhanced cytotoxicity and prolonged survival in vivo after adoptive transfer, and exerted a stronger antitumor immunity against the immunosuppressive IL-10-secreting B16 lung tumors in mice[143]. Injecting a TNF-engineered tumor vaccine into tumors strongly augmented their overall antitumor effectiveness through development of systemic antitumor immunity [144, 145].…”

Section: Tnf and Cancer Therapymentioning

confidence: 99%

Tumor necrosis factor and cancer, buddies or foes?

2008

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Tumor necrosis factor (TNF) is a multifunctional cytokine that plays important roles in diverse cellular events such as cell survival, proliferation, differentiation, and death. As a pro-inflammatory cytokine, TNF is secreted by inflammatory cells, which may be involved in inflammation-associated carcinogenesis. TNF exerts its biological functions through activating distinct signaling pathways such as nuclear factor-κB (NF-κB) and c-Jun N-terminal kinase (JNK). NF-κB is a major cell survival signal that is anti-apoptotic, whereas sustained JNK activation contributes to cell death. The crosstalk between the NF-κB and JNK is involved in determining cellular outcomes in response to TNF. In regard to cancer, TNF is a double-dealer. On one hand, TNF could be an endogenous tumor promoter, because TNF stimulates the growth, proliferation, invasion and metastasis, and tumor angiogenesis of cancer cells. On the other hand, TNF could be a cancer killer. The property of TNF in inducing cancer cell death renders it a potential cancer therapeutic, although much work is needed to reduce its toxicity for systematic TNF administration. Recent studies have focused on sensitizing cancer cells to TNF-induced apoptosis through inhibiting survival signals such as NF-κB, by combined therapy. In this article we provide an overview of the roles of TNF-induced signaling pathways in cancer biology with specific emphasis on carcinogenesis and cancer therapy.

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Section: Tnf and Cancer Therapymentioning

confidence: 99%

Tumor necrosis factor and cancer, buddies or foes?

2008

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“…T cell activation induced expression of α v β3 and α v β5 integrins on cell surface has already been known for quite some time [4]. Although reports of successful RGD-fiber modified virus mediated gene delivery in T cells have been reported, knowledge about viral-replication in the transduced T cells has not yet been addressed [30].…”

Section: Introductionmentioning

confidence: 99%

Enhanced Transduction and Replication of RGD-Fiber Modified Adenovirus in Primary T Cells

et al. 2011

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BackgroundAdenoviruses are often used as vehicles to mediate gene delivery for therapeutic purposes, but their research scope in hematological cells remains limited due to a narrow choice of host cells that express the adenoviral receptor (CAR). T cells, which are attractive targets for gene therapy of numerous diseases, remain resistant to adenoviral infection because of the absence of CAR expression. Here, we demonstrate that this resistance can be overcome when murine or human T cells are transduced with an adenovirus incorporating the RGD-fiber modification (Ad-RGD).Methodology/Principal FindingA luciferase-expressing replication-deficient Ad-RGD infected 3-fold higher number of activated primary T cells than an adenovirus lacking the RGD-fiber modification in vitro. Infection with replication-competent Ad-RGD virus also caused increased cell cycling, higher E1A copy number and enriched hexon antigen expression in both human and murine T cells. Transduction with oncolytic Ad-RGD also resulted in higher titers of progeny virus and enhanced the killing of T cells. In vivo, 35–45% of splenic T cells were transduced by Ad-RGD.ConclusionsCollectively, our results prove that a fiber modified Ad-RGD successfully transduces and replicates in primary T cells of both murine and human origin.

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“…These data suggest that TLR4 deficiency led to decreased platelet activation on tumour cell infusion. Recruitment of immune cells, such as T cells, NK cells, NKT cells and myeloid-derived suppressor cells (MDSCs) can affect the tumour burden in the lung [34][35][36][37] . Therefore, we determined the changes in the composition of immune cell subsets of splenocytes, blood and metastatic tumour foci in the lung in tumour-bearing mice.…”

Section: Experimental Metastasis Is Diminished In Tlr4-deficient Micementioning

confidence: 99%

Platelets promote tumour metastasis via interaction between TLR4 and tumour cell-released high-mobility group box1 protein

et al. 2014

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Increasing evidence suggests that TLR4 expression by tumour cells promotes tumour progression, but it is unclear whether TLR4 is involved in metastasis. Here we show that TLR4 deficiency significantly diminishes experimental lung metastasis without affecting primary tumour growth. Bone marrow transplantation experiment and application of antiplatelet agents in mice demonstrate that TLR4 on platelets plays an important role in metastasis. TLR4 is critical for platelet-tumour cell interaction in vitro. Furthermore, high-mobility group box1 (HMGB1) neutralization attenuates platelet-tumour cell interaction in vitro and metastasis in vivo in a TLR4-dependent manner, indicating that tumour cell-released HMGB1 is the key factor that interacts with TLR4 on platelets and mediates platelet-tumour cell interaction, which promotes metastasis. These findings demonstrate a mechanism by which platelets promote tumour cell metastasis and suggest TLR4, and its endogenous ligand HMGB1 as targets for antimetastatic therapies.

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Engineered CD8+ cytotoxic T cells with fiber-modified adenovirus-mediated TNF-α gene transfection counteract immunosuppressive interleukin-10-secreting lung metastasis and solid tumors

Cited by 11 publications

References 61 publications

Tumor necrosis factor and cancer, buddies or foes?

Tumor necrosis factor and cancer, buddies or foes?

Enhanced Transduction and Replication of RGD-Fiber Modified Adenovirus in Primary T Cells

Platelets promote tumour metastasis via interaction between TLR4 and tumour cell-released high-mobility group box1 protein

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