Oncolytic adenoviruses targeted to Human Papilloma Virus-positive head and neck squamous cell carcinomas

LaRocca, Christopher J.; Han, Joohee; Salzwedel, Amanda O.; Davydova, Julia; Herzberg, Mark C.; Gopalakrishnan, Rajaram; Yamamoto, Masato

doi:10.1016/j.oraloncology.2016.02.014

Cited by 13 publications

(10 citation statements)

References 40 publications

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“…Promoter-based CRAd Lung, prostate, ovarian, pancreatic cancer, adult T cell Leukemia/Lymphoma, glioma, meduloblastoma, sarcomas [69,[209][210][211][212][213][214][215][216][217][218][219][220][221][222] CRAds based on Interaction of essential viral genes withTumor-specific proteins colon, breast, non-small cell lung, head and neck, and pancreatic tumors, cervical carcinoma, glioblastoma, cancers with disturbed Rb pathway [172,[223][224][225][226][227][228] As with genes, several endogenous miRNAs and other lncRNAs can be targeted to enhance the detargeting and retargeting ability of OAdVs [229]. For instance, liver, where most of the OAdV sequestration is observed, overexpresses miRNA122 and miR145.…”

Section: Protein-based Effectorsmentioning

confidence: 99%

Oncolytic Adenoviruses: Strategies for Improved Targeting and Specificity

Hajeri

Sharma

Yamamoto

2020

Cancers

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Cancer is a major health problem. Most of the treatments exhibit systemic toxicity, as they are not targeted or specific to cancerous cells and tumors. Adenoviruses are very promising gene delivery vectors and have immense potential to deliver targeted therapy. Here, we review a wide range of strategies that have been tried, tested, and demonstrated to enhance the specificity of oncolytic viruses towards specific cancer cells. A combination of these strategies and other conventional therapies may be more effective than any of those strategies alone.

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Section: Protein-based Effectorsmentioning

confidence: 99%

Oncolytic Adenoviruses: Strategies for Improved Targeting and Specificity

Hajeri

Sharma

Yamamoto

2020

Cancers

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“…However, currently the administration of oncolytic virus is limited to intratumoral injection, because intravenous administration is easy to produce antibodies against the virus. Therefore, clinical trials of oncolytic viruses are limited to superficial tumors such as head and neck cancer 15 . Due to special anatomical structure of the prostate, viral particle can be accurately injected into prostate cancer lesions guided by ultrasound in phase I clinical trials 16 , 17 .…”

Section: Discussionmentioning

confidence: 99%

Oncolytic Adenovirus Harboring Interleukin-24 Improves Chemotherapy for Advanced Prostate Cancer

Mao¹,

Ding²,

Xu³

et al. 2018

J. Cancer

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Purpose: Oncolytic adenoviruses emerge as new agents for cancer therapy. This study aimed to investigate the synergistic anti-tumor activity of oncolytic adenovirus armed with IL-24 (ZD55-IL-24) and docetaxel (DTX) on advanced prostate cancer in vitro and in vivo.Methods: DU145 prostate cancer cells or nude mice xenografted with DU145 prostate cancer cells were treated by ZD55-IL-24 and DTX alone or in combination.Results: DTX did not affect ZD55-IL-24 replication and IL-24 expression in DU145 cells. In vitro, the combination of ZD55-IL-24 and DTX showed synergistic inhibitory effects on prostate cancer cell viability and invasion. In vivo, ZD55-IL-24 and DTX synergistically inhibited the growth and activated the apoptosis of DU145 xenografts, accompanied by significantly decreased PARP-1 levels and increased caspase-3 and caspase-8 levels as well as decreased CD31 expression.Conclusion: We reported the synergistic anti-tumor efficacy of ZD55-IL-24 and DTX on prostate cancer. Our results suggest that chemotherapy combined with oncolytic adenovirus mediated gene therapy is a promising strategy for the treatment of advanced prostate cancer.

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“…One example in many cancers is a defect in the Retinoblastoma (RB)-E2F pathway, which ultimately allows a virus to replicate as its normally negative regulatory function is absent [ 16 ]. Also, regulatory proteins from certain cancers (such as the human papilloma virus E6 and E7 oncoproteins) can functionally transcomplement missing viral proteins (such those in an adenovirus with E1 deletions) to allow for viral replication [ 21 , 22 ]. No matter the mechanism, a key component of any well-designed vector is the ability to selectively replicate in target cells of interest.…”

Section: Oncolytic Virusesmentioning

confidence: 99%

Oncolytic viruses and checkpoint inhibitors: combination therapy in clinical trials

LaRocca

Warner

2018

Clinical & Translational Med

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106

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Advances in the understanding of cancer immunotherapy and the development of multiple checkpoint inhibitors have dramatically changed the current landscape of cancer treatment. Recent large-scale phase III trials (e.g. PHOCUS, OPTiM) are establishing use of oncolytic viruses as another tool in the cancer therapeutics armamentarium. These viruses do not simply lyse cells to achieve their cancer-killing effects, but also cause dramatic changes in the tumor immune microenvironment. This review will highlight the major vector platforms that are currently in development (including adenoviruses, reoviruses, vaccinia viruses, herpesviruses, and coxsackieviruses) and how they are combined with checkpoint inhibitors. These vectors employ a variety of engineered capsid modifications to enhance infectivity, genome deletions or promoter elements to confer selective replication, and encode a variety of transgenes to enhance anti-tumor or immunogenic effects. Pre-clinical and clinical data have shown that oncolytic vectors can induce anti-tumor immunity and markedly increase immune cell infiltration (including cytotoxic CD8 + T cells) into the local tumor microenvironment. This “priming” by the viral infection can change a ‘cold’ tumor microenvironment into a ‘hot’ one with the influx of a multitude of immune cells and cytokines. This alteration sets the stage for subsequent checkpoint inhibitor delivery, as they are most effective in an environment with a large lymphocytic infiltrate. There are multiple ongoing clinical trials that are currently combining oncolytic viruses with checkpoint inhibitors (e.g. CAPTIVE, CAPRA, and Masterkey-265), and the initial results are encouraging. It is clear that oncolytic viruses and checkpoint inhibitors will continue to evolve together as a combination therapy for multiple types of cancers.

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Oncolytic adenoviruses targeted to Human Papilloma Virus-positive head and neck squamous cell carcinomas

Cited by 13 publications

References 40 publications

Oncolytic Adenoviruses: Strategies for Improved Targeting and Specificity

Oncolytic Adenoviruses: Strategies for Improved Targeting and Specificity

Oncolytic Adenovirus Harboring Interleukin-24 Improves Chemotherapy for Advanced Prostate Cancer

Oncolytic viruses and checkpoint inhibitors: combination therapy in clinical trials

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