Tumor Infection by Oncolytic Reovirus Primes Adaptive Antitumor Immunity

Prestwich, R.; Errington, Fiona; Ilett, Elizabeth J.; Morgan, Rhian; Scott, Karen J.; Kottke, Timothy; Thompson, Jill; Morrison, Ewan E.; Harrington, Kevin; Pandha, Hardev; Selby, Peter J.; Vile, Richard G.; Melcher, Alan

doi:10.1158/1078-0432.ccr-08-0831

Cited by 159 publications

(181 citation statements)

References 48 publications

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“…Native B16 melanoma (B16) and Lewis lung carcinoma (LLC) were purchased from the American Type Culture Collection, whereas ovalbumin (ova)-expressing B16 (B16-ova; ref. Antibodies and reagents used in this study were purchased from different manufacturers as follows: eBioscience: Alexa 488-anti-CD11c, PE-anti-CD86, APCanti-CD40, APC-anti-CD80, PE-anti-mouse MHC class I molecule Kb bound to the peptide SIINFEKL (25-D1.16), unconjugated anti-mouse CD16/32, and unconjugated anti-mouse CD49d; Invitrogen: PE-anti-CD3, Alexa 488-IFN-γ, APC-anti-CD107a, unconjugated anti-mouse CD28, and 5-(and-6)-carboxyfluorescein diacetate (CFSE); BioLegend: PerCp-anti-MHC class II (H-2A/E) and PerCp-anti-CD90.2; BD Biosciences: PerCp-anti-CD8; GenScript: SIINFEKL (ova [257][258][259][260][261][262][263][264] ) and KAVYNFATM (LCMV gp [33][34][35][36][37][38][39][40][41] ) peptides.…”

Section: Reovirus Cell Lines and Reagentsmentioning

confidence: 99%

“…B3Z is a genetically engineered T-cell hybridoma that bears ova-specific TCR and expresses β-galactosidase T-cell proliferation and IFN-γ/CD107a assay Lymphocytes were labeled with 1 μmol/L CFSE (32) and then stimulated with either SIINFEKL, tumor lysate (35), and control LCMV gp [33][34][35][36][37][38][39][40][41] peptide (5 μg/mL)-or UV reovirus [1 multiplicity of infection (MOI)]-pulsed BMDCs or concanavalin A (5 μg/mL), or left unstimulated. After 5 days of incubation, cells were harvested, stained with PE-anti-CD3 antibodies and analyzed.…”

Section: B3z Antigen Presentation Assaymentioning

confidence: 99%

“…Reovirus-initiated cytokine response in vitro has previously been reported (38,39); however, the comprehensive profile of such a response in different immune cell subsets or in vivo is still obscure. Using Antibody-based Quantitative (and Qualitative) Cytokine Array, we evaluated the expression of 60 cytokines following reovirus exposure of BMDCs, lymphocytes, and tumor cells in vitro or immunocompetent and immunocompromised mice in vivo.…”

Section: Reovirus Induces Proinflammation Lymphoid Cell Migration Dmentioning

confidence: 99%

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Reovirus Virotherapy Overrides Tumor Antigen Presentation Evasion and Promotes Protective Antitumor Immunity

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Marcato

Pan

et al. 2010

Molecular Cancer Therapeutics

105

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Tumor-associated immunosuppressive strategies, such as lack of tumor antigen recognition and failure of lymphocyte activation and homing, resist the development of tumor-specific immunity and hamper the immune response-mediated elimination of cancerous cells. In this report, we show that reovirus virotherapy overrides such a tumor immune evasion and establishes clinically meaningful antitumor immunity capable of protecting against subsequent tumor challenge. Reovirus-mediated destruction of tumor cells facilitates the recognition of tumor antigens by promoting the display of otherwise inaccessible tumorspecific immunogenic peptides on the surface of dendritic cells (DC). Furthermore, on exposure to reovirus, DCs produce IL-1α, IL-1β, IL-6, IL-12p40/70, IL-17, CD30L, eotaxin, GM-CSF, KC, MCP-1, MCP-5, M-CSF, MIG, MIP-1α, RANTES, TNF-α, VCAM-1, VSGF, CXCL-16, AXL, and MCP-2; undergo maturation; and migrate into the tumor microenvironment along with CD8 T cells. These reovirus-activated DCs also acquire the capacity to prime tumor antigen-specific transgenic T cells in vitro and intrinsic antitumor T-cell response in vivo. Further, reovirus virotherapy augments the efficacy of DC-or T cell-based anticancer immunotherapies and synergistically enhances the survival in tumor-bearing mice. Most importantly, antitumor cellular immune responses initiated during reovirus oncotherapy protect the host against subsequent tumor challenge in a reovirus-independent but antigen-dependent manner. These reovirus oncotherapy-initiated antitumor immune responses represent an anticancer therapeutic entity that can maintain a long-term cancer-free health even after discontinuation of therapy.

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Section: Reovirus Cell Lines and Reagentsmentioning

confidence: 99%

Section: B3z Antigen Presentation Assaymentioning

confidence: 99%

Section: Reovirus Induces Proinflammation Lymphoid Cell Migration Dmentioning

confidence: 99%

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Reovirus Virotherapy Overrides Tumor Antigen Presentation Evasion and Promotes Protective Antitumor Immunity

Gujar

Marcato

Pan

et al. 2010

Molecular Cancer Therapeutics

105

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“…23,42 Infecting tumors with viruses induces antitumor immunity through tyrosinase-related protein 2 and interleukin 12. 43 Moreover, indirect tumor cell killing is induced by the activation of cytokine production and host antitumor immunity. 23,42 Virusadherent lymphocytes become a stimulus for IFN secretion and lead to suppression of tumor growth.…”

Section: Antitumor Efficacy Of Herpes Simplex Virus a Kanzaki Et Almentioning

confidence: 99%

“…43,44 It is thought that long-term antitumor immune memory is initiated by this response. 45 Therefore, although we administered HSV-adherent tumor antigen-specific lymphocytes only once, 40% of the treated mice were completely cured.…”

Section: Antitumor Efficacy Of Herpes Simplex Virus a Kanzaki Et Almentioning

confidence: 99%

Antitumor efficacy of oncolytic herpes simplex virus adsorbed onto antigen-specific lymphocytes

et al. 2012

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Although several studies have reported that locally administering oncolytic viruses effectively targets malignancies, the efficacy of systemically administered oncolytic viruses is restricted. Recently, however, it was reported that systemic administration of oncolytic vesicular stomatitis virus adsorbed onto antigen-specific lymphocytes was effective against malignancies. We hypothesized that intravenously administering such virus might have significant potential in treatment of the malignant tumors. We adsorbed oncolytic herpes simplex virus-1 mutant R3616 onto lymphocytes harvested from mice with acquired antitumor immunity. We administered adsorbed R3616 to peritoneally disseminated tumors and analyzed the efficacy of this treatment. Mice administered adsorbed R3616 survived significantly longer than mice administered R3616 adsorbed onto non-specific lymphocytes, or mice administered either virus or tumor antigen-specific lymphocytes alone. In this context, herpes oncolytic virus is a promising treatment not only for primary lesions, but also for multiple metastasizing lesions. This treatment strategy may become one of the most effective methods for systemic virus delivery.

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The role of viruses in cancer development versus cancer therapy: An oncological perspective

et al. 2023

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Despite great medical advances, oncological research is still looking for novel therapeutic approaches due to the limitation of conventional therapeutic agents. Virotherapy is one of these new emerging therapeutic approaches that attract attention with their widespread applications. Virotherapy use lives oncolytic viruses or genetically engineered viruses that selectively infect the tumor cells, replicate, and disrupt the cancerous cells that also induce their anticancer activity by stimulating the host antitumor immune response. Moreover, viruses are widely used as target delivery vectors for specifically delivering different genes, therapeutic agents, and immune‐stimulating agents. In addition to having antitumor activity by themselves in combination with conventional therapeutic agents like immune therapy and chemotherapy, Virotherapy agents also elicit promising outcomes. Therefore, in addition to their promising result in monotherapy use, virotherapy agents can also be used in combination with conventional cancer therapy, epigenetic modulators, and even microRNAs without any cross‐resistance, which allows the patient not to be deprived of her routine medicine. Still, this combination therapy reduces the adverse effect of the conventional therapies. All together suggest that virotherapy agents as novel potential agents in the field of cancer therapy.

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Tumor Infection by Oncolytic Reovirus Primes Adaptive Antitumor Immunity

Cited by 159 publications

References 48 publications

Reovirus Virotherapy Overrides Tumor Antigen Presentation Evasion and Promotes Protective Antitumor Immunity

Reovirus Virotherapy Overrides Tumor Antigen Presentation Evasion and Promotes Protective Antitumor Immunity

Antitumor efficacy of oncolytic herpes simplex virus adsorbed onto antigen-specific lymphocytes

The role of viruses in cancer development versus cancer therapy: An oncological perspective

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