Triple Combination of Oncolytic Herpes Simplex Virus-1 Vectors Armed with Interleukin-12, Interleukin-18, or Soluble B7-1 Results in Enhanced Antitumor Efficacy

Ino, Yasushi; Saeki, Yoshinaga; Fukuhara, Hiroshi; Todo, Tomoki

doi:10.1158/1078-0432.ccr-05-1494

Cited by 91 publications

(89 citation statements)

References 47 publications

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“…Oncolytic herpes viral therapy in GBM xenografts PC Huszthy et al For GBMIII lesions in the later-effects study (Figure 3i), the median proliferative index in plaques was 16 10.73). The noninfected regions in vector-treated animals had significantly higher proliferation rate than the levels found in saline-injected control animals (Po0.001), indicating a possible compensatory response to the reduced proliferation in plaques.…”

Section: Proliferation Rates In G207-infected Plaquesmentioning

confidence: 93%

“…7 Therefore, subsequent developments of HSV-1-based glioma therapy have focused on ways to enhance antitumor efficacy. 8 Two main strategies have been followed: modifying the vectors by deleting the immunoattenuating genes coded for by the virus, to allow enhanced immunorecognition of vector-infected cells, 9 or, by inserting immunostimulatory or therapeutic transgenes, [10][11][12][13] as well as by combining the vectors with other clinical treatment forms such as chemotherapy 14 or irradiation. 15 In neuro-oncology, the validity of experimental data obtained from preclinical evaluation of potential clinical therapies has been compromised by the widespread use of tumor-cell-line-based animal models.…”

Section: Introductionmentioning

confidence: 99%

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Cellular effects of oncolytic viral therapy on the glioblastoma microenvironment

et al. 2009

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The objective of the present study was to evaluate the cellular effects of the oncolytic HSV-1 based vector, G207, on the tumor microenvironment. We established progressively growing intracerebral xenografts in athymic nude rats generated from three different human GBM surgical specimens. The lesions were identified by MRI and subsequently injected with a concentrated vector stock. The animals were killed 10 or 30 days after G207 injection and the tumors were quantitatively evaluated for virus-induced changes in proliferation, apoptosis and vascularity. Moreover, we assessed vector spread as well as the infiltration pattern of CD68-positive inflammatory cells. In all G207-injected lesions, immunostaining identified widespread regions of viral infection and replication (plaques). Proliferation indices were significantly lower, whereas apoptotic counts were significantly elevated in plaques as compared with that in non-infected areas of the same lesions, as well as in corresponding control xenografts. Furthermore, there was a significant decline in the number of blood vessels in the plaques and the vascular area fractions were reduced. CD68-positive inflammatory cells accumulated in the plaques. The present study highlights the favorable cellular responses to G207 treatment seen from a clinical viewpoint, such as reduced tumor cell proliferation, more frequent events of tumor cell death and a strongly attenuated tumor vascular compartment. However, our results suggest that transduction of a significant volume of tumor tissue is essential, as these beneficial changes were only observed in areas of active viral replication, leaving non-transduced tumor tissues unaffected.

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Section: Proliferation Rates In G207-infected Plaquesmentioning

confidence: 93%

Section: Introductionmentioning

confidence: 99%

Cellular effects of oncolytic viral therapy on the glioblastoma microenvironment

et al. 2009

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“…18) expressed from vaccinia virus or GM-CSF (19) expressed from herpes simplex virus] has shown great promise in clinical trials. In addition, preclinical reports of other viruses modified to express cytokines were able to confer an increase in their therapeutic efficacy in several tumor models (20)(21)(22)(23)(24)(25)(26)(27). In this regard, we developed several NDV vectors carrying GM-CSF, tumor necrosis factor (TNF)-a, IFN-g, or IL-2 and tested them for increased therapeutic efficacy.…”

Section: Introductionmentioning

confidence: 99%

Use of Reverse Genetics to Enhance the Oncolytic Properties of Newcastle Disease Virus

Vigil¹,

Park²,

Martinez³

et al. 2007

Cancer Research

148

153

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Naturally occurring strains of Newcastle disease virus (NDV) have shown oncolytic therapeutic efficacy in preclinical studies and are currently in clinical trials. Here, we have evaluated the possibility to enhance the cancer therapeutic potential of NDV by means of reverse genetics. Mice bearing s.c. implanted CT26 tumors were treated with intratumoral (i.t.) injections of a recombinant NDV modified to contain a highly fusogenic F protein. These treated mice exhibited significant reduction in tumor development compared with mice treated with the unmodified virus. Furthermore, mice in a CT26 metastatic tumor model treated with an i.v. injection of the genetically engineered NDV exhibited prolonged survival compared with wild-type control virus. In addition, we examined whether the oncolytic properties of NDV could be improved by expression of immunostimulatory molecules. In this regard, we engineered several NDVs to express granulocyte macrophage colony-stimulating factor, IFN-;, interleukin 2 (IL-2), or tumor necrosis factor A, and evaluated their therapeutic potential in an immunocompetent colon carcinoma tumor model. Mice bearing s.c. CT26 tumors treated with i.t. injections of recombinant NDV expressing IL-2 showed dramatic reductions in tumor growth, with a majority of the mice undergoing complete and long-lasting remission. Our data show the use of reverse genetics to develop enhanced recombinant NDV vectors as effective therapeutic agents for cancer treatment. [Cancer Res 2007;67(17):8285-92]

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“…Using the HSVQuik system, we also created oncolytic HSV-1 armed with IL-12, IL-18 or soluble B7-1. 19 All of these armed HSV-1 demonstrated replicative capabilities similar to the parental virus in vitro. The in vivo efficacy was tested in A/J mice harboring subcutaneous tumors of syngeneic and poorly immunogenic Neuro2a neuroblastoma.…”

confidence: 98%

“Armed” oncolytic herpes simplex viruses for brain tumor therapy

Todo¹

2008

Cell Adhesion & Migration

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Triple Combination of Oncolytic Herpes Simplex Virus-1 Vectors Armed with Interleukin-12, Interleukin-18, or Soluble B7-1 Results in Enhanced Antitumor Efficacy

Cited by 91 publications

References 47 publications

Cellular effects of oncolytic viral therapy on the glioblastoma microenvironment

Cellular effects of oncolytic viral therapy on the glioblastoma microenvironment

Use of Reverse Genetics to Enhance the Oncolytic Properties of Newcastle Disease Virus

“Armed” oncolytic herpes simplex viruses for brain tumor therapy

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