Clinical development directions in oncolytic viral therapy

Eager, Robert M; Nemunaitis, John

doi:10.1038/cgt.2011.7

Cited by 93 publications

(82 citation statements)

References 154 publications

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“…OVs represent a promising approach as anti-cancer therapeutics; however preclinical and clinical studies have demonstrated limited efficacy of OVs alone, prompting effort to combine them with other anti-cancer agents to improve their antitumor effects (Eager & Nemunaitis 2011. We have previously demonstrated that the oncolytic adenoviruses dl1520 and dl922-947 are active against ATC in vitro and in vivo (Libertini et al 2007(Libertini et al , 2008.…”

Section: Discussionmentioning

confidence: 99%

“…With respect to classical anti-cancer drugs, OVs present several advantages: tumor-selective replication with amplification of the input dose, stimulation of anti-tumoral immune responses, and relatively few mild side effects when administered to human patients. Also, the development of cross-resistance is unlikely because their mechanism of action is independent of conventional anti-cancer therapeutics (Eager & Nemunaitis 2011. A number of OVs, such as the vaccinia virus GLV-1h68 (Lin et al 2008b) and the oncolytic attenuated herpes virus G207 (Lin et al 2008a), have shown promising effects against ATC cells in preclinical studies.…”

Section: Introductionmentioning

confidence: 99%

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Ionizing radiation enhances dl922–947-mediated cell death of anaplastic thyroid carcinoma cells

Abagnale¹,

Libertini²,

Volpe³

et al. 2013

Endocrine-Related Cancer

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dl922-947 is an oncolytic adenovirus potentially suitable for the treatment of aggressive localized tumors, such as anaplastic thyroid carcinoma (ATC). In this study, we have analyzed the effects of dl922-947 in combination with ionizing radiations, testing different schedules of administration and observing synergistic effects only when ATC cells were irradiated 24 h prior to viral infection. Cells undergoing combined treatment exhibited a marked increase in cell death and viral replication, suggesting that irradiation blocks cells in a more permissive state for viral life cycle. We also show that dl922-947 triggers a DNA damage response, characterized by mobilization of the MRN complex (composed by Mre11-Rad50-Nbs1), accumulation of gH2AX, and activation of the checkpoint kinases ataxia telangiectasia mutated (ATM) and Chk1. Based on these observations, we speculate that the DNA damage response acts as a cellular protective mechanism to hinder viral infection and replication. To confirm this hypothesis, we demonstrate that the ATM inhibitor KU55933 increased the oncolytic activity of dl922-947 and its replication. Finally, we validate the potential therapeutic use of this approach by showing in vivo that the combined treatment slows tumor xenograft growth more potently than either irradiation or infection alone.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Ionizing radiation enhances dl922–947-mediated cell death of anaplastic thyroid carcinoma cells

Abagnale¹,

Libertini²,

Volpe³

et al. 2013

Endocrine-Related Cancer

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“…antiadenovirus immunity is vigorous, many groups have made it even more so by generating replication-competent adenoviruses as therapeutic strategies to treat cancer, that is, to enlist the antiadenovirus immunity in killing cancer cells (Short and Curiel, 2009;Eager and Nemunaitis, 2011;Alemany, 2012;Cerullo et al, 2012;Russell et al, 2012;Choi and Yun, 2013). Third, we and others have leveraged the potent immunity against the adenovirus to create vaccines against the transgene (Krause and Worgall, 2011) or by inserting the antigen in the capsid (Lasaro and Ertl, 2009;Thacker et al, 2009;Matthews, 2011).…”

Section: Crystalmentioning

confidence: 99%

Adenovirus: The First EffectiveIn VivoGene Delivery Vector

2014

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“…One or more  sequences with 400 base pair (bp) join the L and S segments. Gene-modified HSV includes inactivation of ICP6 gene and deletion of -34.5 [12]. ICP6 encodes the large subunit of ribonucleotide reductase, which is essential for viral DNA replication.…”

Section: An Overview Of Hsvmentioning

confidence: 99%

Advance in herpes simplex viruses for cancer therapy

Liu

Dai

You

et al. 2013

Sci. China Life Sci.

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Oncolytic virotherapy is an attractive approach that uses live viruses to selectively kill cancer cells. Oncolytic viruses can be genetically engineered to induce cell lyses through virus replication and cytotoxic protein expression. Herpes simplex virus (HSV) has become one of the most widely clinically used oncolytic agent. Various types of HSV have been studied in basic or clinical research. Combining oncolytic virotherapy with chemotherapy or radiotherapy generally produces synergic action with unclear molecular mechanisms. Arming HSV with therapeutic transgenes is a promising strategy and can be used to complement conventional therapies. As an efficient gene delivery system, HSV has been successfully used to deliver various immunomodulatory molecules. Arming HSV with therapeutic genes merits further investigation for potential clinical application.

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Clinical development directions in oncolytic viral therapy

Cited by 93 publications

References 154 publications

Ionizing radiation enhances dl922–947-mediated cell death of anaplastic thyroid carcinoma cells

Ionizing radiation enhances dl922–947-mediated cell death of anaplastic thyroid carcinoma cells

Adenovirus: The First EffectiveIn VivoGene Delivery Vector

Advance in herpes simplex viruses for cancer therapy

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