Literature DB >> 21792179

Precise scheduling of chemotherapy primes VEGF-producing tumors for successful systemic oncolytic virotherapy.

Timothy Kottke1, John Chester, Elizabeth Ilett, Jill Thompson, Rosa Diaz, Matt Coffey, Peter Selby, Gerard Nuovo, Jose Pulido, Debabrata Mukhopadhyay, Hardev Pandha, Kevin Harrington, Alan Melcher, Richard Vile.   

Abstract

We have previously reported that a burst of vascular endothelial growth factor (VEGF) signaling to tumor-associated endothelium induces a proviral state, during which systemically delivered oncolytic reovirus can replicate in endothelium, thereby inducing immune-mediated vascular collapse and significant antitumor therapy. Using chimeric receptors, we show here that induction of the proviral state proceeds through VEGFR2, but not VEGFR1, signaling in endothelial cells. In contrast, innate immune activation by reovirus-exposed endothelial cells was predominantly through VEGFR1. By screening conventional chemotherapies for their ability to induce similar effects in combination with reovirus both in vitro and in vivo, we observed that the proviral state could also be induced in endothelial cells exposed to VEGF during rebound from paclitaxel-mediated inhibition of VEGF signaling. We translated these in vitro findings in vivo by careful scheduling of paclitaxel chemotherapy with systemic virotherapy, neither of which alone had therapeutic effects against B16 tumors. Systemic availability of reovirus during endothelial cell recovery from paclitaxel treatment allowed for endothelial replication of the virus, immune-mediated therapy, and tumor cures. Therefore, careful scheduling of combination viro- and chemotherapies, which preclinical testing suggests are individually ineffective against tumor cells, can lead to rational new clinical protocols for systemic treatments with oncolytic viruses.

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Year:  2011        PMID: 21792179      PMCID: PMC3188745          DOI: 10.1038/mt.2011.147

Source DB:  PubMed          Journal:  Mol Ther        ISSN: 1525-0016            Impact factor:   11.454


  50 in total

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8.  Tyrosine residues 951 and 1059 of vascular endothelial growth factor receptor-2 (KDR) are essential for vascular permeability factor/vascular endothelial growth factor-induced endothelium migration and proliferation, respectively.

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  17 in total

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3.  In vitro screen of a small molecule inhibitor drug library identifies multiple compounds that synergize with oncolytic myxoma virus against human brain tumor-initiating cells.

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Review 4.  Oncolytic virotherapy for urological cancers.

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5.  Subversion of NK-cell and TNFα Immune Surveillance Drives Tumor Recurrence.

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6.  Mutated BRAF Emerges as a Major Effector of Recurrence in a Murine Melanoma Model After Treatment With Immunomodulatory Agents.

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7.  Cytokine conditioning enhances systemic delivery and therapy of an oncolytic virus.

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8.  Detecting and targeting tumor relapse by its resistance to innate effectors at early recurrence.

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9.  Trial watch: Oncolytic viruses for cancer therapy.

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10.  Gemcitabine enhances the efficacy of reovirus-based oncotherapy through anti-tumour immunological mechanisms.

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