Cellular effects of oncolytic viral therapy on the glioblastoma microenvironment

Huszthy, Peter C.; Immervoll, Heike; Wang, J; Goplen, Dorota; Miletić, Hrvoje; Eide, Geir Egil; Bjerkvig, Rolf

doi:10.1038/gt.2009.130

Cited by 20 publications

(21 citation statements)

References 46 publications

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“…53 Some oncolytic herpes viruses reduce apoptosis; 45,46,54 whereas others enhance apoptosis. 43,44,47 The effect of oncolytic herpes viruses on apoptosis is strain specific and depends on the underlying genetic variation. Defects in the US3 arm or gamma 34.5 may induce apoptosis in infected cells; this may explain why gamma 34.5 deleted viruses such as G207 induce apoptosis.…”

Section: X400 X400mentioning

confidence: 99%

“…[39][40][41][42] The effects of oncolytic herpes viruses on apoptosis are controversial: apoptosis is elevated upon viral treatment in some studies, 43,44 but reduced in others. 45,46 Some have argued that induction of premature apoptosis is not a desirable feature of oncolytic viral treatment; 47 instead, reducing or delaying apoptosis may enhance viral penetration of the tumor, another determinant of the potency of an oncolytic virus.…”

Section: Introductionmentioning

confidence: 99%

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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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Section: X400 X400mentioning

confidence: 99%

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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“…The ␥ 1 34.5-deleted HSV G207, which also contains an inactivating insertion of lacZ within the U L 39 gene encoding ICP6 (ribonucleotide reductase heavy chain), has demonstrated efficacy in vivo against brain tumors in a number of syngeneic and xenogeneic models of GBM (1,2,15,16,34), neuroblastoma (52,53,55), and meningioma (59). The similar virus HSV1716 is also deleted for ␥ 1 34.5 but retains the U L 39 gene (26,32) and has demonstrated efficacy in two different brain tumor models (19,24).…”

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confidence: 99%

Preclinical Evaluation of a Genetically Engineered Herpes Simplex Virus Expressing Interleukin-12

Markert

Cody

Parker

et al. 2012

J Virol

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Herpes simplex virus 1 (HSV-1) mutants that lack the γ 1 34.5 gene are unable to replicate in the central nervous system but maintain replication competence in dividing cell populations, such as those found in brain tumors. We have previously demonstrated that a γ 1 34.5-deleted HSV-1 expressing murine interleukin-12 (IL-12; M002) prolonged survival of immunocompetent mice in intracranial models of brain tumors. We hypothesized that M002 would be suitable for use in clinical trials for patients with malignant glioma. To test this hypothesis, we (i) compared the efficacy of M002 to three other HSV-1 mutants, R3659, R8306, and G207, in murine models of brain tumors, (ii) examined the safety and biodistribution of M002 in the HSV-1-sensitive primate Aotus nancymae following intracerebral inoculation, and (iii) determined whether murine IL-12 produced by M002 was capable of activating primate lymphocytes. Results are summarized as follows: (i) M002 demonstrated superior antitumor activity in two different murine brain tumor models compared to three other genetically engineered HSV-1 mutants; (ii) no significant clinical or magnetic resonance imaging evidence of toxicity was observed following direct inoculation of M002 into the right frontal lobes of A. nancymae ; (iii) there was no histopathologic evidence of disease in A. nancymae 1 month or 5.5 years following direct inoculation; and (iv) murine IL-12 produced by M002 activates A. nancymae lymphocytes in vitro . We conclude that the safety and preclinical efficacy of M002 warrants the advancement of a Δγ 1 34.5 virus expressing IL-12 to phase I clinical trials for patients with recurrent malignant glioma.

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“…This effect can be countered through the administration of thrombospondin-derived peptides. In models of glioblastoma, cases where oncolytic virus infection results in an anti-angiogenic response, adjacent virus-free areas have been shown to upregulate angiogenesis (Huszthy et al, 2010). Furthermore, increases in tumor angiogenesis can facilitate virus-induced inflammatory responses.…”

Section: The Tumor Microenvironmentmentioning

confidence: 99%

Herpes Simplex Type 1 for Use in Cancer Gene Therapy: Looking Backward to Move Forward

Cuddington¹,

Mossman²

2011

Viral Gene Therapy

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Cellular effects of oncolytic viral therapy on the glioblastoma microenvironment

Cited by 20 publications

References 46 publications

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

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

Preclinical Evaluation of a Genetically Engineered Herpes Simplex Virus Expressing Interleukin-12

Herpes Simplex Type 1 for Use in Cancer Gene Therapy: Looking Backward to Move Forward

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