&lt;p&gt;Virus–Receptor Interactions and Virus Neutralization: Insights for Oncolytic Virus Development&lt;/p&gt;

Jayawardena, Nadishka; Poirier, John T.; Burga, Laura N.; Bostina, Mihnea

doi:10.2147/ov.s186337

Cited by 31 publications

(32 citation statements)

References 127 publications

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“…Other determinants of emerging infectious agents include cell tropism, ability to circumvent innate immune responses, and antigenic immunodominance, among others. Many viruses enter cells via one or more cell receptors ( Figure 4 ) ( Dai et al., 2020 ; Jayawardena et al., 2020 ); some infect different cells via different receptors, while some cell receptors may be entry points for multiple different types of viruses. The situation is extraordinarily complex from the point of view of both virus and host, with a bewildering array of receptors, alternate receptors, and co-receptors and of countless viruses able to utilize them, reflecting that “viruses have deep evolutionary roots in the cellular world” ( Baranowski et al., 2001 ).…”

Section: Variables In Disease Emergence: the Agent Host And Environmentioning

confidence: 99%

Emerging Pandemic Diseases: How We Got to COVID-19

Morens

Fauci

2020

Cell

534

350

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Infectious diseases prevalent in humans and animals are caused by pathogens that once emerged from other animal hosts. In addition to these established infections, new infectious diseases periodically emerge. In extreme cases they may cause pandemics such as COVID-19; in other cases, dead-end infections or smaller epidemics result. Established diseases may also re-emerge, for example by extending geographically or by becoming more transmissible or more pathogenic. Disease emergence reflects dynamic balances and imbalances, within complex globally distributed ecosystems comprising humans, animals, pathogens, and the environment. Understanding these variables is a necessary step in controlling future devastating disease emergences.

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Section: Variables In Disease Emergence: the Agent Host And Environmentioning

confidence: 99%

Emerging Pandemic Diseases: How We Got to COVID-19

Morens

Fauci

2020

Cell

534

350

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“…There are many cases where anti-viral immunity already exists because most OVs used in anti-cancer therapy are human pathogens that are abundant in the environment. Moreover, repeated OV administration not only induces anti-tumor immunity but also triggers anti-viral immunity [ 82 , 90 ]. Anti-viral immunity can suppress viral replication, facilitate viral clearance, and attenuate anti-tumor activity in immunocompetent patients [ 25 , 82 ].…”

Section: Current Limitations Of Ovs For Cancer Treatmentmentioning

confidence: 99%

“…For example, neutralizing antibodies against Vaccinia virus target H3L envelope protein and interrupt viral-host fusion [ 91 ]. In the case of adenovirus, pre-existing neutralizing antibodies reduced the anti-tumor efficacy of oncolytic adenovirus [ 90 ]. Furthermore, T-VEC administration is limited to intratumoral injection because of high anti-HSV-1 antibody prevalence in humans [ 90 , 92 ].…”

Section: Current Limitations Of Ovs For Cancer Treatmentmentioning

confidence: 99%

“…In the case of adenovirus, pre-existing neutralizing antibodies reduced the anti-tumor efficacy of oncolytic adenovirus [ 90 ]. Furthermore, T-VEC administration is limited to intratumoral injection because of high anti-HSV-1 antibody prevalence in humans [ 90 , 92 ]. In addition to pre-existing neutralizing antibodies, anti-viral immunity can also be mediated by the complement system, anti-viral cytokines, and non-specific uptake by off-target organs [ 82 ].…”

Section: Current Limitations Of Ovs For Cancer Treatmentmentioning

confidence: 99%

“…In addition to pre-existing neutralizing antibodies, anti-viral immunity can also be mediated by the complement system, anti-viral cytokines, and non-specific uptake by off-target organs [ 82 ]. Therefore, to tackle anti-viral immunity, multiple strategies, including genetic manipulation of OV, cytokines, immunomodulators, nanoparticles, and the depletion of neutralizing antibodies, have been explored [ 82 , 83 , 90 ]. On the other hand, there are several conflicting reports suggesting anti-viral immunity could sometimes be beneficial for anti-tumor immunity because anti-viral immunity can recruit anti-tumor immune cells into the TME and reverse the immunosuppressive TME [ 5 , 27 ].…”

Section: Current Limitations Of Ovs For Cancer Treatmentmentioning

confidence: 99%

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Combination Immunotherapy Using Oncolytic Virus for the Treatment of Advanced Solid Tumors

Chon

Kim

2020

IJMS

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Oncolytic virus (OV) is a new therapeutic strategy for cancer treatment. OVs can selectively infect and destroy cancer cells, and therefore act as an in situ cancer vaccine by releasing tumor-specific antigens. Moreover, they can remodel the tumor microenvironment toward a T cell-inflamed phenotype by stimulating widespread host immune responses against the tumor. Recent evidence suggests several possible applications of OVs against cancer, especially in combination with immune checkpoint inhibitors. In this review, we describe the molecular mechanisms of oncolytic virotherapy and OV-induced immune responses, provide a brief summary of recent preclinical and clinical updates on this rapidly evolving field, and discuss a combinational strategy that is able to overcome the limitations of OV-based monotherapy.

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