Neuroblastomas vary widely in their sensitivities to herpes simplex virotherapy unrelated to virus receptors and susceptibility

Py, Wang; Swain, Hayley M.; Kunkler, Anne L.; Cy, Chen; Hutzen, Brian; Arnold, Michael A.; Streby, Keri A.; Collins, Margaret H.; DiPasquale, Betsy Ann; Stanek, Joseph; Conner, Joe; Kuppevelt, Toin H. Van; Grandi, Paola; Cripe, Timothy P.

doi:10.1038/gt.2015.105

Cited by 29 publications

(31 citation statements)

References 30 publications

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“…The in vitro HSV entry molecule expression and cytotoxicity data suggest that SARC-45 may be more susceptible than SARC-28 to infection with M002; however, the virus replicated equally in both cell lines after 24 hr of infection, and entry receptor molecule expression does not always correlate with higher viral entry. 23 Our in vivo studies examining the response to a single dose of M002 in immunocompromised mice bearing SARC-28 and SARC-45 in an immunoprivileged location confirmed the significant oncolytic effect of M002 in the absence of an adaptive host immune system. Previous studies demonstrated that human alveolar and embryonal rhabdomyosarcoma and renal sarcoma cell lines with high expression of CD111 were sensitive to in vitro killing by oHSV.…”

Section: Discussionsupporting

confidence: 65%

Newly Characterized Murine Undifferentiated Sarcoma Models Sensitive to Virotherapy with Oncolytic HSV-1 M002

Ring

Moore

et al. 2017

Molecular Therapy - Oncolytics

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Despite advances in conventional chemotherapy, surgical techniques, and radiation, outcomes for patients with relapsed, refractory, or metastatic soft tissue sarcomas are dismal. Survivors often suffer from lasting morbidity from current treatments. New targeted therapies with less toxicity, such as those that harness the immune system, and immunocompetent murine sarcoma models to test these therapies are greatly needed. We characterized two new serendipitous murine models of undifferentiated sarcoma (SARC-28 and SARC-45) and tested their sensitivity to virotherapy with oncolytic herpes simplex virus 1 (HSV-1). Both models expressed high levels of the primary HSV entry molecule nectin-1 (CD111) and were susceptible to killing by interleukin-12 (IL-12) producing HSV-1 M002 in vitro and in vivo. M002 resulted in a significant intratumoral increase in effector CD4+ and CD8+ T cells and activated monocytes, and a decrease in myeloid-derived suppressor cells (MDSCs) in immunocompetent mice. Compared to parent virus R3659 (no IL-12 production), M002 resulted in higher CD8:MDSC and CD8:T regulatory cell (Treg) ratios, suggesting that M002 creates a more favorable immune tumor microenvironment. These data provide support for clinical trials targeting sarcomas with oncolytic HSV-1. These models provide an exciting opportunity to explore combination therapies for soft tissue sarcomas that rely on an intact immune system to reach full therapeutic potential.

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Section: Discussionsupporting

confidence: 65%

Newly Characterized Murine Undifferentiated Sarcoma Models Sensitive to Virotherapy with Oncolytic HSV-1 M002

Ring

Moore

et al. 2017

Molecular Therapy - Oncolytics

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“…However, T‐01 had no detectable effect on HLE and JHH‐5 cells, likely because of the relatively low levels of T‐01 replication (Figure ). It cannot negate the possibility that the entry efficiency of T‐01 into cells and/or the expression levels of HSV receptors on cell lines used were involved in the cytopathic activities of T‐01 in addition to the levels of T‐01 replication . Such information may help to elucidate why some tumors are highly sensitive to oHSV, and may lead to methods for selecting patients with the most sensitive tumors in oHSV therapy.…”

Section: Discussionmentioning

confidence: 99%

Third‐generation oncolytic herpes simplex virus inhibits the growth of liver tumors in mice

et al. 2018

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Multimodality therapies are used to manage patients with hepatocellular carcinoma (HCC), although advanced HCC is incurable. Oncolytic virus therapy is probably the next major breakthrough in cancer treatment. The third‐generation oncolytic herpes simplex virus type 1 (HSV‐1) T‐01 kills tumor cells without damaging the surrounding normal tissues. Here we investigated the antitumor effects of T‐01 on HCC and the host's immune response to HCC cells. The cytopathic activities of T‐01 were tested in 14 human and 1 murine hepatoma cell line in vitro. In various mouse xenograft models, HuH‐7, KYN‐2, PLC/PRF/5 and HepG2 human cells and Hepa1‐6 murine cells were used to investigate the in vivo efficacy of T‐01. T‐01 was cytotoxic to 13 cell lines (in vitro). In mouse xenograft models of subcutaneous, orthotopic and peritoneal tumor metastasis in athymic mice (BALB/c nu/nu), the growth of tumors formed by the human HCC cell lines and hepatoblastoma cell line was inhibited by T‐01 compared with that of mock‐inoculated tumors. In a bilateral Hepa1‐6 subcutaneous tumor model in C57BL/6 mice, the growth of tumors inoculated with T‐01 was inhibited, as was the case for contralateral tumors. T‐01 also significantly reduced tumor growth. T‐01 infection significantly enhanced antitumor efficacy via T cell‐mediated immune responses. Results demonstrate that a third‐generation oncolytic HSV‐1 may serve as a novel treatment for patients with HCC.

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“…There is abundant evidence that HSV-1 mutants deficient in the ␥ 1 34.5 gene have oncolytic activities. This has been shown for tumors, including in the brain, colon, ovarian, breast, liver, and skin, in immunodeficient as well as in immunocompetent preclinical models (24)(25)(26)(27)(28)(29)(30)(31). However, the antitumor outcomes vary widely.…”

mentioning

confidence: 98%

“…For example, HSV1716 is highly potent against hepatocellular carcinoma (30). With respect to neuroblastomas, HSV1716 exhibits activities from a complete response in the CHP-134 model to a mild effect in the SK-N-AS model (31). The underlying events are complex, but the nature of virus-host interactions seems a determinant.…”

mentioning

confidence: 99%

Selective Editing of Herpes Simplex Virus 1 Enables Interferon Induction and Viral Replication That Destroy Malignant Cells

Xing

2019

J Virol

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Oncolytic herpes simplex virus 1 (HSV-1), devoid of the γ134.5 gene, exerts antitumor activities. However, the oncolytic effects differ, ranging from pronounced to little responses. Although viral and host factors are involved, much remains to be deciphered. Here we report that engineered HSV-1 ΔN146, bearing amino acids 147 to 263 of γ134.5, replicates competently in and lyses malignant cells refractory to the γ134.5 null mutant. Upon infection, ΔN146 precludes phosphorylation of translation initiation factor eIF2α (α subunit of eukaryotic initiation factor 2), ensuring viral protein synthesis. On the other hand, ΔN146 activates interferon (IFN) regulatory factor 3 (IRF3) and IFN expression, known to prime immunity against virus and tumor. Nevertheless, ΔN146 exhibits sustained replication even exposed to exogenous IFN-α. In a 4T1 tumor model, ΔN146 markedly reduces tumor growth and metastasis formation. This coincides with viral replication or T cell infiltration in primary tumors. ΔN146 is undetectable in normal tissues in vivo. Targeted HSV-1 editing results in a unique antineoplastic agent that enables inflammation without major interference of viral growth within tumor cells. IMPORTANCE Oncolytic herpes simplex virus 1 is a promising agent for cancer immunotherapy. Due to a complex virus-host interaction, less is clear about what viral signature(s) constitutes a potent oncolytic backbone. Through molecular or genetic dissection, we showed that selective editing of the γ134.5 gene enables viral replication in malignant cells, activation of transcription factor IRF3, and subsequent induction of type I IFN. This translates into profoundly reduced primary tumor growth and metastasis burden in an aggressive breast carcinoma model in vivo. Our work reveals a distinct oncolytic platform that is amendable for further development.

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Neuroblastomas vary widely in their sensitivities to herpes simplex virotherapy unrelated to virus receptors and susceptibility

Cited by 29 publications

References 30 publications

Newly Characterized Murine Undifferentiated Sarcoma Models Sensitive to Virotherapy with Oncolytic HSV-1 M002

Newly Characterized Murine Undifferentiated Sarcoma Models Sensitive to Virotherapy with Oncolytic HSV-1 M002

Third‐generation oncolytic herpes simplex virus inhibits the growth of liver tumors in mice

Selective Editing of Herpes Simplex Virus 1 Enables Interferon Induction and Viral Replication That Destroy Malignant Cells

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