4.5 Article

Oncolytic parvoviruses: from basic virology to clinical applications

期刊

VIROLOGY JOURNAL
卷 12, 期 -, 页码 -

出版社

BMC
DOI: 10.1186/s12985-014-0223-y

关键词

Oncolytic parvoviruses; Parvovirus-based cancer virotherapy; Parvovirus-based oncolytic vectors; Parvovirus-based combination therapy; Rodent protoparvovirus; Glioblastoma multiforme; Oncolytic virotherapy clinical trial

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资金

  1. Oryx GmbH
  2. Federal Ministry of Education and Research (BMBF)
  3. Helmholz Association in the framework of the Deutsches Krebsforschungszentrum/Canceropole du Grand-Est Joint Programme in Applied Tumour Virology
  4. Deutsche Krebshilfe [109826]

向作者/读者索取更多资源

Accumulated evidence gathered over recent decades demonstrated that some members of the Parvoviridae family, in particular the rodent protoparvoviruses H-1PV, the minute virus of mice and LuIII have natural anticancer activity while being nonpathogenic to humans. These studies have laid the foundations for the launch of a first phase I/IIa clinical trial, in which the rat H-1 parvovirus is presently undergoing evaluation for its safety and first signs of efficacy in patients with glioblastoma multiforme. After a brief overview of the biology of parvoviruses, this review focuses on the studies which unraveled the antineoplastic properties of these agents and supported their clinical use as anticancer therapeutics. Furthermore, the development of novel parvovirus-based anticancer strategies with enhanced specificity and efficacy is discussed, in particular the development of second and third generation vectors and the combination of parvoviruses with other anticancer agents. Lastly, we address the key challenges that remain towards a more rational and efficient use of oncolytic parvoviruses in clinical settings, and discuss how a better understanding of the virus life-cycle and of the cellular factors involved in virus infection, replication and cytotoxicity may promote the further development of parvovirus-based anticancer therapies, open new prospects for treatment and hopefully improve clinical outcome.

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