Host Lymphodepletion Enhances the Therapeutic Activity of an Oncolytic Vaccinia Virus Expressing 4-1BB Ligand

Kim, Hong Sung; Kim‐Schulze, Seunghee; Kim, Dae Won; Kaufman, Howard L.

doi:10.1158/0008-5472.can-09-2522

Cited by 50 publications

(34 citation statements)

References 43 publications

(52 reference statements)

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“…For example, expression of the ligands of TNF receptor superfamily such as OX40L, 4-1BBL, and GITRL by has been demonstrated to enhance the efficacy of adenovirus and vaccinia vectors delivered intratumorally (Andarini et al, 2004;Calmels et al, 2005;Kim, Kim-Schulze, Kim, & Kaufman, 2009). Most of the studies demonstrated that such viruses could induce stronger infiltration of immune cells into the virus-injected tumors; however, the question remained whether this was merely a reflection of an enhanced antiviral immune response and whether this would translate into a more effective systemic antitumor immunity.…”

Section: Oncolytic Virusesmentioning

confidence: 99%

The New Era of Cancer Immunotherapy

Khalil¹,

Budhu²,

Gasmi³

et al. 2015

Advances in Cancer Research

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Section: Oncolytic Virusesmentioning

confidence: 99%

The New Era of Cancer Immunotherapy

Khalil¹,

Budhu²,

Gasmi³

et al. 2015

Advances in Cancer Research

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“…These antigen-presenting cells in turn stimulate a Th1 response, which promotes T-cell-based tumor killing. 18,19 …”

Section: Viral Selectionmentioning

confidence: 99%

Immune cells: more than simple carriers for systemic delivery of oncolytic viruses

Eisenstein¹,

Chen²,

Pan³

2014

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Oncolytic virotherapy on its own has numerous drawbacks, including an inability of the virus to actively target tumor cells and systemic toxicities at the high doses necessary to effectively treat tumors. Addition of immune cell-based carriers of oncolytic viruses holds promise as a technique in which oncolytic virus can be delivered directly to tumors in smaller and less toxic doses. Interestingly, the cell carriers themselves have also demonstrated antitumor effects, which can be augmented further by tailoring the appropriate oncolytic virus to the appropriate cell type. This review discusses the multiple factors that go into devising an effective, cell-based delivery system for oncolytic viruses.

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“…These studies concluded that administration of naïve and early effector T cells, in combination with a lymphodepleting pretreatment regimen, g c cytokine administration, and vaccination, resulted in the eradication of established tumors (18)(19)(20). A conditioning treatment of mice (e.g., sublethal irradiation) prior to iPS cell transfer or cytokine treatment (IL-2 or IL-15) may benefit iPS cell-based therapies.…”

Section: Adoptive Transfer Of Tcr Gene-transduced Ips Cells Prevents mentioning

confidence: 99%

In Vivo Programming of Tumor Antigen-Specific T Lymphocytes from Pluripotent Stem Cells to Promote Cancer Immunosurveillance

et al. 2011

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Adoptive T-cell immunotherapy has garnered wide attention, but its effective use is limited by the need of multiple ex vivo manipulations and infusions that are complex and expensive. In this study, we show how highly reactive antigen (Ag)-specific CTLs can be generated from induced pluripotent stem (iPS) cells to provide an unlimited source of functional CTLs for adoptive immunotherapy. iPS cell-derived T

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Host Lymphodepletion Enhances the Therapeutic Activity of an Oncolytic Vaccinia Virus Expressing 4-1BB Ligand

Cited by 50 publications

References 43 publications

The New Era of Cancer Immunotherapy

The New Era of Cancer Immunotherapy

Immune cells: more than simple carriers for systemic delivery of oncolytic viruses

In Vivo Programming of Tumor Antigen-Specific T Lymphocytes from Pluripotent Stem Cells to Promote Cancer Immunosurveillance

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