A novel translational approach for human malignant pleural mesothelioma: heparanase-assisted dual virotherapy

Watanabe, Yuichi; Kojima, Toru; Kagawa, Shunsuke; Uno, Futoshi; Hashimoto, Yuichi; Kyo, Satoru; Mizuguchi, Hiroyuki; Tanaka, Noriaki; Kawamura, Hikaru; Ichimaru, Daiju; Urata, Yasuo; Fujiwara, Toshiyoshi

doi:10.1038/onc.2009.415

Cited by 31 publications

(26 citation statements)

References 33 publications

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“…When tested in highly metastatic tumor models neither relaxin-induced MMP expression nor expression of heparanase, hyaluronidase, or decorin increased metastasis. On the contrary, coadministration or expression of these enzymes with oncolytic virus reduced metastasis in the models tested Ganesh et al, 2008;Choi et al, 2010;Watanabe et al, 2010). Still, this risk must always be considered when examining the therapeutic potential of agents that degrade the ECM in solid tumors.…”

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confidence: 91%

“…The intratumoral administration of a replicating oncolytic adenovirus along with a nonreplicating adenovirus expressing heparanase resulted in increased viral spread within tumor spheroids, reduced tumor growth, and a significant improvement in survival in a malignant plural human mesothelioma mouse model in vivo (Watanabe et al, 2010). In general, targeting the ECM is an effective strategy used to increase viral diffusion throughout solid tumors.…”

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confidence: 99%

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Strategies to Enhance Viral Penetration of Solid Tumors

2011

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The efficient delivery of viral vectors to tumors is an active area of investigation. A number of barriers exist that must be overcome to achieve good penetration of vectors into tumors and distribution of their effects throughout the tumor mass. Replicating oncolytic viruses have the advantage of being able to amplify the initial dose, but progeny virus are prevented from spreading because of a dense mass of tightly packed cells with a dense extracellular matrix, admixed normal stromal cells, and high interstitial pressure. Although intratumoral injection may ensure initial delivery the distribution achieved by intravenous administration may be superior and come with beneficial bystander damage to the tumor vasculature. Strategies to enhance intravenous delivery and subsequent spread of these vectors within tumors are being developed by a number of groups. Achieving the goal of efficient penetration and spread of viruses within solid tumors is a necessary prerequisite to significant improvements in virus-vectored therapy of solid tumors.

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confidence: 91%

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confidence: 99%

Strategies to Enhance Viral Penetration of Solid Tumors

2011

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“…43,45,50,51 It has been previously investigated that chondroitin sulfates and proteoglycans/glycosaminoglycans that exist within the pleural effusion interact with the vector in the solution and not with the target cells and therefore inhibit the treatment. 52,53 Although, an enzymatic pre-treatment was proposed, further investigation of the molecular pathways of MPE discouraged this approach.…”

Section: Discussionmentioning

confidence: 99%

Management of malignant pleural effusion by suicide gene therapy in advanced stage lung cancer: a case series and literature review

et al. 2012

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“…These viruses are used either alone, for their direct cytotoxic effects on the tumor [33], [3], or in combination, enhancing tumor susceptibility to a secondary chemotherapy [50], [55], [11],[48], [57], [58]. These viruses are usually variants of naturally occurring viruses.…”

Section: Medical Applications Of Evolutionmentioning

confidence: 99%

Controlling the evolution of resistance

Luo¹,

Cannon²,

Hernandez³

et al. 2011

Journal of Process Control

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Evolution has long been understood as the driving force for many problems of medical interest. The evolution of drug resistance in HIV and bacterial infections is recognized as one of the most significant emerging problems in medicine. In cancer therapy, the evolution of resistance to chemotherapeutic agents is often the differentiating factor between effective therapy and disease progression or death. Interventions to manage the evolution of resistance have, up to this point, been based on steady-state analysis of mutation and selection models. In this paper, we review the mathematical methods applied to studying evolution of resistance in disease. We present a broad review of several classical applications of mathematical modeling of evolution, and review in depth two recent problems which demonstrate the potential for interventions which exploit the dynamic behavior of resistance evolution models. The first problem addresses the problem of sequential treatment failures in HIV; we present a review of our recent publications addressing this problem. The second problem addresses a novel approach to gene therapy for pancreatic cancer treatment, where selection is used to encourage optimal spread of susceptibility genes through a target tumor, which is then eradicated during a second treatment phase. We review the recent in Vitro laboratory work on this topic, present a new mathematical model to describe the treatment process, and show why model-based approaches will be necessary to successfully implement this novel and promising approach.

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A novel translational approach for human malignant pleural mesothelioma: heparanase-assisted dual virotherapy

Cited by 31 publications

References 33 publications

Strategies to Enhance Viral Penetration of Solid Tumors

Strategies to Enhance Viral Penetration of Solid Tumors

Management of malignant pleural effusion by suicide gene therapy in advanced stage lung cancer: a case series and literature review

Controlling the evolution of resistance

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