A High-throughput Pharmacoviral Approach Identifies Novel Oncolytic Virus Sensitizers

Diallo, Jean-Simon; Bœuf, Fabrice Le; Lai, Frances W.; Cox, Julie A.; Vähä‐Koskela, Markus; Abdelbary, Hesham; MacTavish, Heather; Waite, Katherine; Falls, Theresa; Wang, Jenny; Brown, Ryan; Blanchard, Jan; Brown, Eric D.; Kirn, David H.; Hiscott, John; Atkins, Harry; Lichty, Brian D.; Bell, John C.

doi:10.1038/mt.2010.67

Cited by 90 publications

(82 citation statements)

References 30 publications

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“…A highthroughput screening approach 14 identified seven approved drugs that have microtubule-destabilizing activity among 15 previously unknown compounds found to enhance VSVD51-mediated oncolysis. The compounds, their drug class and structures are listed in Supplementary Table 1.…”

Section: Resultsmentioning

confidence: 99%

Microtubule disruption synergizes with oncolytic virotherapy by inhibiting interferon translation and potentiating bystander killing

et al. 2015

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In this study, we show that several microtubule-destabilizing agents used for decades for treatment of cancer and other diseases also sensitize cancer cells to oncolytic rhabdoviruses and improve therapeutic outcomes in resistant murine cancer models. Drug-induced microtubule destabilization leads to superior viral spread in cancer cells by disrupting type I IFN mRNA translation, leading to decreased IFN protein expression and secretion. Furthermore, microtubule-destabilizing agents specifically promote cancer cell death following stimulation by a subset of infection-induced cytokines, thereby increasing viral bystander effects. This study reveals a previously unappreciated role for microtubule structures in the regulation of the innate cellular antiviral response and demonstrates that unexpected combinations of approved chemotherapeutics and biological agents can lead to improved therapeutic outcomes.

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Section: Resultsmentioning

confidence: 99%

Microtubule disruption synergizes with oncolytic virotherapy by inhibiting interferon translation and potentiating bystander killing

et al. 2015

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“…Red fluorescence protein-tagged VSV-M⌬51 (Indiana serotype) was a gift from J. Bell (University of Ottawa, Ottawa, Canada) (11). VSV was propagated in BHK-21 cells, and titers were determined by plaque assay in the same cells (62).…”

Section: Methodsmentioning

confidence: 99%

Virus-Activated Interferon Regulatory Factor 7 Upregulates Expression of the Interferon-Regulated BST2 Gene Independently of Interferon Signaling

Bego

Mercier

Cohen

2012

J Virol

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bBST-2/tetherin is an interferon (IFN)-inducible host restriction factor that inhibits the release of many enveloped viruses and functions as a negative-feedback regulator of IFN production by plasmacytoid dendritic cells. Currently, mechanisms underlying BST2 transcriptional regulation by type I IFN remain largely unknown. Here, we demonstrate that the BST2 promoter is a secondary target of the IFN cascade and show that a single IRF binding site is sufficient to render this promoter responsive to IFN-␣. Interestingly, expression of IRF-1 or virus-activated forms of IRF-3 and IRF-7 stimulated the BST2 promoter even under conditions where type I IFN signaling was inhibited. Indeed, vesicular stomatitis virus could directly upregulate BST-2 during infection of mouse embryonic fibroblasts through a process that required IRF-7 but was independent from the type I IFN cascade; however, in order to achieve optimal BST-2 induction, the type I IFN cascade needed to be engaged through activation of IRF-3. Furthermore, using human peripheral blood mononuclear cells, we show that BST-2 upregulation is part of an early intrinsic immune response since TLR8 and TLR3 agonists, known to trigger pathways that mediate activation of IRF proteins, could upregulate BST-2 prior to engagement of the type I IFN pathway. Collectively, our findings reveal that BST2 is activated by the same signals that trigger type I IFN production, outlining a regulatory mechanism ensuring that production of type I IFN and expression of a host restriction factor involved in the IFN negative-feedback loop are closely coordinated.

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“…One key characteristic of oncolytic viruses is that they can be genetically modified to express reporter transgenes which makes it possible to visualize the infection of tissues by microscopy or bio-luminescence imaging 6,7 . This offers a unique advantage since it is possible to infect tissues from patients ex vivo prior to therapy in order to ascertain the likelihood of successful oncolytic virotherapy 8 . To this end, it is critical to appropriately sample tissue to compensate for tissue heterogeneity and assess tissue viability, particularly prior to infection 9 .…”

Section: Introductionmentioning

confidence: 99%

<em>Ex Vivo</em> Infection of Live Tissue with Oncolytic Viruses

Diallo

Roy

Abdelbary

et al. 2011

JoVE

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A High-throughput Pharmacoviral Approach Identifies Novel Oncolytic Virus Sensitizers

Cited by 90 publications

References 30 publications

Microtubule disruption synergizes with oncolytic virotherapy by inhibiting interferon translation and potentiating bystander killing

Microtubule disruption synergizes with oncolytic virotherapy by inhibiting interferon translation and potentiating bystander killing

Virus-Activated Interferon Regulatory Factor 7 Upregulates Expression of the Interferon-Regulated BST2 Gene Independently of Interferon Signaling

<em>Ex Vivo</em> Infection of Live Tissue with Oncolytic Viruses

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