Literature DB >> 24322333

Maraba virus as a potent oncolytic vaccine vector.

Jonathan G Pol1, Liang Zhang1, Byram W Bridle2, Kyle B Stephenson3, Julien Rességuier1, Stephen Hanson1, Lan Chen1, Natasha Kazdhan1, Jonathan L Bramson1, David F Stojdl4, Yonghong Wan1, Brian D Lichty5.   

Abstract

The rhabdovirus Maraba has recently been characterized as a potent oncolytic virus. In the present study, we engineered an attenuated Maraba strain, defined as MG1, to express a melanoma-associated tumor antigen. Its ability to mount an antitumor immunity was evaluated in tumor-free and melanoma tumor-bearing mice. Alone, the MG1 vaccine appeared insufficient to prime detectable adaptive immunity against the tumor antigen. However, when used as a boosting vector in a heterologous prime-boost regimen, MG1 vaccine rapidly generated strong antigen-specific T-cell immune responses. Once applied for treating syngeneic murine melanoma tumors, our oncolytic prime-boost vaccination protocol involving Maraba MG1 dramatically extended median survival and allowed complete remission in more than 20% of the animals treated. This work describes Maraba virus MG1 as a potent vaccine vector for cancer immunotherapy displaying both oncolytic activity and a remarkable ability to boost adaptive antitumor immunity.

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Year:  2013        PMID: 24322333      PMCID: PMC3916044          DOI: 10.1038/mt.2013.249

Source DB:  PubMed          Journal:  Mol Ther        ISSN: 1525-0016            Impact factor:   11.454


  29 in total

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2.  Recent advances in vesicular stomatitis virus-based oncolytic virotherapy: a 5-year update.

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Review 3.  Trial watch: DNA-based vaccines for oncological indications.

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Review 9.  Going viral with cancer immunotherapy.

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Review 10.  The emerging role of oncolytic virus therapy against cancer.

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