Multimutated Herpes Simplex Virus G207 Is a Potent Inhibitor of Angiogenesis

Činátl, Jindřich; Michaelis, Martin; Driever, Pablo Hernáiz; Činátl, Jaroslav; Hraběta, Jan; Suhan, Tatyana; Doerr, Hans Wilhelm; Vogel, Jens‐Uwe

doi:10.1593/neo.04265

Cited by 47 publications

(32 citation statements)

References 41 publications

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“…Furthermore, as the FGF signaling pathway is critical to tumor growth and angiogenesis, the enhanced potency should be seen in both FGF-secreting and FGF-nonsecreting tumors, thus broadening the application of the vector. Of note, our data support previous publications that oncolytic HSV mutants with deletions in c34.5 and/or ICP6 have antiangiogenic activities by themselves, inhibiting capillary tube formation in vitro and in vivo and replicating in tumor endothelial cells but not in normal vasculature in vivo (41,42). We showed that G47D is a potent antiangiogenic virus; it significantly reduced endothelial cell proliferation by direct cell killing as well as HUVEC migration in a Transwell coculture system, presumably due to a reduction in angiogenic factors secreted by infected tumor cells.…”

Section: Discussionsupporting

confidence: 91%

Dominant-Negative Fibroblast Growth Factor Receptor Expression Enhances Antitumoral Potency of Oncolytic Herpes Simplex Virus in Neural Tumors

Liu

Zhang²,

Fukuhara³

et al. 2006

Clinical Cancer Research

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Purpose: Oncolytic herpes simplex viruses (HSV) appear to be a promising platform for cancer therapy. However, efficacy as single agents has thus far been unsatisfactory. Fibroblast growth factor (FGF) signaling is important for the growth and migration of endothelial and tumor cells. Here, we examine the strategy of arming oncolytic HSV with a dominant-negative FGF receptor (dnFGFR) that targets the FGF signaling pathway. Experimental Design: A mouse Nf1:p53 malignant peripheral nerve sheath tumor (MPNST) cell line expressing dnFGFR was generated by transfection. The effects of dnFGFR expression on cell growth and migration in vitro and tumor formation in vivo were determined. The dnFGFR transgene was then inserted into oncolytic HSV G47D using a bacterial artificial chromosome construction system. Antitumoral and antiangiogenic activities of bG47D-dnFGFR were examined. Results: MPNST 61E4 cells expressing dnFGFR grew less well than parental control cells. bG47D-dnFGFR showed enhanced killing of both tumor (human U87 glioma and F5 malignant meningioma cells and murine MPNST 61E4 and 37-3-18-4 cells) and proliferating endothelial cells (human umbilical vascular endothelial cell and Py-4-1) in vitro compared with the control vector bG47D-empty without inhibiting viral replication. In vivo, bG47D-dnFGFR was more efficacious than its nonexpressing parent bG47D-empty at inhibiting tumor growth and angiogenesis in both human U87 glioma and mouse 37-3-18-4 MPNST tumors in nude mice. Conclusions: By using multiple therapeutic mechanisms, including destruction of both tumor cells and tumor endothelial cells, an oncolytic HSV encoding dnFGFR enhances antitumor efficacy. This strategy can be applied to other oncolytic viruses and for clinical translation.

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Section: Discussionsupporting

confidence: 91%

Dominant-Negative Fibroblast Growth Factor Receptor Expression Enhances Antitumoral Potency of Oncolytic Herpes Simplex Virus in Neural Tumors

Liu

Zhang²,

Fukuhara³

et al. 2006

Clinical Cancer Research

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“…11,45,46 In one study, mice bearing rhabdomyosarcoma xenografts were injected intratumorally with G207. 45 Eight days post injection, endothelial structures were found to be absent in the vector-injected lesions, and the authors detected enveloped viral particles in endothelialcell cytoplasms. 45 Other studies showed that G207 enhanced mean blood vessel densities, a finding explained by reduction of the intratumoral levels of the angiogenesis inhibitors thrombospondin-1 and 2.…”

Section: Effects On the Tumor Vascular Compartmentmentioning

confidence: 99%

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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“…Preclinical data regarding herpetic stromal keratitis has revealed enhanced angiogenesis upon infection with wild-type HSV. 25 The situation is more complicated for oncolytic viruses: some well-designed studies indicate that such viruses may have antiangiogenic properties, 24,26 whereas other researchers have reported enhanced angiogenesis occurring via a range of mechanisms. [27][28][29] There are many attempts to engineer viruses to express antiangiogenic molecules.…”

Section: Introductionmentioning

confidence: 99%

Impact of novel oncolytic virus HF10 on cellular components of the tumor microenviroment in patients with recurrent breast cancer

et al. 2011

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Oncolytic viruses are a promising method of cancer therapy, even for advanced malignancies. HF10, a spontaneously mutated herpes simplex type 1, is a potent oncolytic agent. The interaction of oncolytic herpes viruses with the tumor microenvironment has not been well characterized. We injected HF10 into tumors of patients with recurrent breast carcinoma, and sought to determine its effects on the tumor microenvironment. Six patients with recurrent breast cancer were recruited to the study. Tumors were divided into two groups: saline-injected (control) and HF10-injected (treatment). We investigated several parameters including neovascularization (CD31) and tumor lymphocyte infiltration (CD8, CD4), determined by immunohistochemistry, and apoptosis, determined by terminal deoxynucleotidyl transferase dUTP nick end labeling assay. Median apoptotic cell count was lower in the treatment group (P ¼ 0.016). Angiogenesis was significantly higher in treatment group (P ¼ 0.032). Count of CD8-positive lymphocytes infiltrating the tumors was higher in the treatment group (P ¼ 0.008). We were unable to determine CD4-positive lymphocyte infiltration. An effective oncolytic viral agent must replicate efficiently in tumor cells, leading to higher viral counts, in order to aid viral penetration. HF10 seems to meet this criterion; furthermore, it induces potent antitumor immunity. The increase in angiogenesis may be due to either viral replication or the inflammatory response.

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Multimutated Herpes Simplex Virus G207 Is a Potent Inhibitor of Angiogenesis

Cited by 47 publications

References 41 publications

Dominant-Negative Fibroblast Growth Factor Receptor Expression Enhances Antitumoral Potency of Oncolytic Herpes Simplex Virus in Neural Tumors

Dominant-Negative Fibroblast Growth Factor Receptor Expression Enhances Antitumoral Potency of Oncolytic Herpes Simplex Virus in Neural Tumors

Cellular effects of oncolytic viral therapy on the glioblastoma microenvironment

Impact of novel oncolytic virus HF10 on cellular components of the tumor microenviroment in patients with recurrent breast cancer

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