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2015 Fiscal Year Final Research Report

Development of replication-selective oncolytic viral vector using modified mammalian orthoreovirus

Research Project

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Project/Area Number 25860340
Research Category

Grant-in-Aid for Young Scientists (B)

Allocation TypeMulti-year Fund
Research Field Virology
Research InstitutionOsaka University

Principal Investigator

KANAI YUTA  大阪大学, 微生物病研究所, 特任講師(常勤) (80506501)

Co-Investigator(Renkei-kenkyūsha) Kobayashi Takeshi  大阪大学, 微生物病研究所 感染症国際研究センター ウイルス複製研究グループ, 特任准教授 (90324847)
Research Collaborator Kawagishi Takahiro  大阪大学, 微生物病研究所 感染症国際研究センター ウイルス複製研究グループ, 学振特別研究員
Matsuura Yoshiharu  大阪大学, 微生物病研究所 分子ウイルス分野, 教授 (50157252)
Okamoto Toru  大阪大学, 微生物病研究所 分子ウイルス分野, 助教 (80628595)
Project Period (FY) 2013-04-01 – 2016-03-31
Keywordsレオウイルス / 癌 / 遺伝子治療
Outline of Final Research Achievements

Mammalian Reovirus (MRV) has important capacity that MRV show selective oncolytic activity in cancer cells. Currently, wild type T3D-C strain, which displays significant oncolytic activity, is developed as viral oncolytic agent.
To develop improved oncolytic MRV reagent, we established reverse genetics system for T3D-C strain, the known strongest oncolytic strain. We generated recombinant RGD-MRV which has integrin-interactive RGD motif in MRV sigma1 protein to enable infection to MRV-resistant cancer cells via MRV receptor independent manner. This RGD-MRV exhibited enhanced infectivity and oncolysis of reovirus-resistant cancer cell. Next, we have generated reporter-MRV which express exogenous Luciferase (NanoLuc) transgene. Infection and replication site of Nanoluc-MRV in mice model could be monitored by in vivo imaging system (IVIS). Further, when NanoLuc-MRV were injected intravenously to human cancer xenograft mice, IVIS revealed that NanoLuc-MRV selectively infected in tumor.

Free Research Field

ウイルス学

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Published: 2017-05-10  

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