Safety Studies on Intravenous Administration of Oncolytic Recombinant Vesicular Stomatitis Virus in Purpose-Bred Beagle Dogs

LeBlanc, Amy K.; Naik, Shruthi; Galyon, Gina D.; Jenks, Nathan J.; Steele, Mike; Peng, Kah Whye; Federspiel, Mark J.; Donnell, Robert; Russell, Stephen J.

doi:10.1089/humc.2013.165

Cited by 45 publications

(62 citation statements)

References 16 publications

(22 reference statements)

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“…Using VSVs encoding type I and type III IFNs Several recent pre-clinical studies have shown that VSVIFNb and VSV-IFNb-NIS (additionally expresses the NIS to track virus spread) are oncoselective and safe in a variety of tumour and animal models [24,[27][28][29][30][31]. Although mice and rats continue to serve as the most commonly used animal models for VSV-based OV therapy, a recent study evaluated the safety of intravenously administered VSV-IFNb-NIS in purpose-bred beagle dogs.…”

Section: Improving Oncoselectivity and Safetymentioning

confidence: 99%

“…dose of 10 10 TCID50 was well-tolerated by dogs. Furthermore, no infectious virus was detectable in plasma, urine or buccal swabs at any tested doses [29]. Importantly, VSV-IFNb-NIS is currently in several phase I clinical trials in the USA: against refractory solid tumours (see details at ClinicalTrials.gov trial NCT02923466), stage IV or recurrent endometrial cancer (trial NCT03120624), and relapsed or refractory multiple myeloma, acute myeloid leukemia or T-cell lymphoma (trial NCT03017820).…”

Section: Improving Oncoselectivity and Safetymentioning

confidence: 99%

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Recent advances in vesicular stomatitis virus-based oncolytic virotherapy: a 5-year update

Felt

Grdzelishvili

2017

Journal of General Virology

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Oncolytic virus (OV) therapy is an anti-cancer approach that uses viruses that preferentially infect, replicate in and kill cancer cells. Vesicular stomatitis virus (VSV, a rhabdovirus) is an OV that is currently being tested in the USA in several phase I clinical trials against different malignancies. Several factors make VSV a promising OV: lack of pre-existing human immunity against VSV, a small and easy to manipulate genome, cytoplasmic replication without risk of host cell transformation, independence of cell cycle and rapid growth to high titres in a broad range of cell lines facilitating large-scale virus production. While significant advances have been made in VSV-based OV therapy, room for improvement remains. Here we review recent studies (published in the last 5 years) that address 'old' and 'new' challenges of VSV-based OV therapy. These studies focused on improving VSV safety, oncoselectivity and oncotoxicity; breaking resistance of some cancers to VSV; preventing premature clearance of VSV; and stimulating tumour-specific immunity. Many of these approaches were based on combining VSV with other therapeutics. This review also discusses another rhabdovirus closely related to VSV, Maraba virus, which is currently being tested in Canada in phase I/II clinical trials.

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Section: Improving Oncoselectivity and Safetymentioning

confidence: 99%

Section: Improving Oncoselectivity and Safetymentioning

confidence: 99%

Recent advances in vesicular stomatitis virus-based oncolytic virotherapy: a 5-year update

Felt

Grdzelishvili

2017

Journal of General Virology

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“…Safety studies in research beagles before the start of the canine trial indicated that the maximal tolerated dose (MTD) in dogs is 10 10 TCID 50 (50% tissue culture infective dose) of VSV-hIFNb-NIS or VSVcIFNb-NIS. 6 At 10 · MTD (10 11 TCID 50 ), the doselimiting toxicity is severe hepatotoxicity with elevations in transaminases and prolongation of partial thromboplastin time (PTT), requiring euthanasia of the animal. Intensive pharmacokinetics studies showed a rapid increase in VSV-nucleocapsid (N) RNA in the blood from 10 min to 3 hr after virus infusion (end of acute-phase monitoring).…”

Section: Introductionmentioning

confidence: 99%

Safety Studies in Tumor and Non-Tumor-Bearing Mice in Support of Clinical Trials Using Oncolytic VSV-IFNβ-NIS

Zhang

Steele

Jenks

et al. 2016

Human Gene Therapy Clinical Development

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“…Additionally, the virus has been administered intravenously to purpose bred research hounds where the maximal tolerated dose was determined to be 10 10 TCID 50 (dose-limiting toxicity was mildly elevated transaminases). 15 VSV-IFNβ-NIS is active against a broad spectrum of tumors of differing tissue origins and tumor response is typically not associated with significant toxicities. For example, in immunocompetent mice with large subcutaneous 5TGM1 myeloma tumors, an intravenous dose of 3 × 10 8 TCID 50 VSV-murine IFNβ-NIS can result in sustained complete remission and induction of tumorspecific memory T cells that protect the mice from new tumor cell challenge.…”

Section: Introductionmentioning

confidence: 99%

Robust Oncolytic Virotherapy Induces Tumor Lysis Syndrome and Associated Toxicities in the MPC-11 Plasmacytoma Model

et al. 2016

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Safety Studies on Intravenous Administration of Oncolytic Recombinant Vesicular Stomatitis Virus in Purpose-Bred Beagle Dogs

Cited by 45 publications

References 16 publications

Recent advances in vesicular stomatitis virus-based oncolytic virotherapy: a 5-year update

Recent advances in vesicular stomatitis virus-based oncolytic virotherapy: a 5-year update

Safety Studies in Tumor and Non-Tumor-Bearing Mice in Support of Clinical Trials Using Oncolytic VSV-IFNβ-NIS

Robust Oncolytic Virotherapy Induces Tumor Lysis Syndrome and Associated Toxicities in the MPC-11 Plasmacytoma Model

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